BIODEGRADABLE DRUG DELIVERY FOR HYDROPHOBIC COMPOSITIONS

Abstract
A biodegradable drug delivery compositions comprising a triblock copolymer containing a polyester and a polyethylene glycol and a diblock copolymer containing a polyester and an end-capped polyethylene glycol, as well as at least one pharmaceutically active principle or hydrophobic active principle such as medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine is disclosed.
Description
FIELD OF THE INVENTION

The present invention relates to biodegradable drug delivery compositions comprising a triblock copolymer containing a polyester and a polyethylene glycol and a diblock copolymer containing a polyester and an end-capped polyethylene glycol, as well as a pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine. The ratio of triblock copolymer to diblock copolymer in this formulation is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1. Methods for producing these biodegradable drug compositions using organic solvents are also disclosed.


BACKGROUND OF THE PRESENT INVENTION

Drug delivery systems such as diblock and triblock copolymers have been used to deliver a variety of drugs and are generally formulated to deliver specific drugs whether they are hydrophobic drugs or hydrophilic drugs. Depending on the drug solubility these drug formulations differ in polymer concentrations, types of polymers utilized, molecular weights of the polymers and solvents used in the formulations.


Also the type of environment in which the drug is delivered is an important consideration in formulating a drug delivery system. Thus, there exist drug delivery compositions that are prepared using temperature sensitive polymers, phase sensitive polymers, pH sensitive polymers and photosensitive polymers. See, for example, K. Al-Tahami and J. Singh “Smart Polymer Based Delivery Systems for Peptide and Proteins,” Recent Patents on Drug Delivery & Formulation, 1: pages: 65-71 Bentham Science Publishers, L T D. 2007.


U.S. Pat. No. 6,592,899 describes a PLA/PLGA oligomer combined with a block copolymer for enhancing the solubility of a hydrophobic drug into a hydrophilic environment. More specifically this polymer composition has a polyester oligomer having a molecular weight of between 400 and 10,000 daltons and a biodegradable AB-type, ABA-type or BAB type block copolymer. The hydrophobic A part is a polyester, while the hydrophilic B part is a polyethylene glycol having a molecular weight of between 2,400 and 4,999 daltons. This polymeric composition is soluble in an aqueous environment.


U.S. Pat. No. 6,541,033 describes a sustained release pharmaceutical composition based on thermosensitive, biodegradable hydrogels, consisting of a block copolymer of PLA or PLGA and PEG, for the sustained delivery of biologically active agents, such as leptin. The sustained release is for a period of a week or more and preferably up to one month.


Hydrogels containing triblock copolymers are described in U.S. Pat. No. 6,350,812. These hydrogels retain water weight at least equal to the water weight of the copolymer and are soft hydrogels.


U.S. Pat. No. 7,875,677 provides micelle-forming compositions comprising a hydrophobic drug, a biocompatible block copolymer, which has a hydrophilic protein comprising a polyethylene oxide and a hydrophobic portion having a polyester and a biocompatible water soluble polymer, wherein the water soluble polymer is present in a sufficient amount to make the micelle-forming composition injectable.


It is well known in the art that poorly water soluble or hydrophobic drugs often result in slow drug absorption leading to inadequate and variable bioavailability and gastrointestinal mucosal toxicity. Hence, formulating hydrophobic drugs is a challenge well known in this art.


None of the patents nor the literature cited above describes drug delivery compositions that are injectable, in situ forming and are biodegradable and turn into solid implants when injected into the body and deliver pharmaceutically hydrophobic active principles. The biodegradable drug compositions of the present invention comprise triblock copolymers and diblock copolymers formulated in such a manner that the diblock copolymer serves as a reservoir while the triblock copolymer acts as a frame in the formulations and increases the lifespan of the diblock copolymer.


Furthermore, the biodegradable drug delivery compositions of the present invention can be long acting formulations, which reduce the initial burst release of the drug and modulate the release rate of the drug or hydrophobic drug over time. This phenomenon is illustrated in the flattening of the drug release curves.


SUMMARY OF THE INVENTION

The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 in said biodegradable drug composition; and (c) at least one pharmaceutically active principle.


The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically active principle.


The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle.


The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine.


The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 in said biodegradable drug composition; and (c) at least one pharmaceutically active principle.


The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically active principle.


The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle.


The present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine.


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically active principle.


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically active principle.


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically hydrophobic active principle.


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine.


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically active principle


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically active principle


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically hydrophobic active principle


A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition and wherein the PEG in the diblock is end-capped; and (c) at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine.


In yet another aspect a biodegradable drug delivery composition is provided, which comprises: (a) a biodegradable triblock copolymer present in an amount of 3% to 45% (w %/w %) of the total composition having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer present in an amount of 8.0% to 50% (w %/w %) of the total composition having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 in said biodegradable drug composition and wherein the PEG in the diblock is end capped and (c) at least one pharmaceutically active principle is present in an amount of 1% to 20% (w %/w %) of the total composition or the at least one pharmaceutically active principle is present in an amount of 1 to 200 mg/ml.


In yet another aspect a biodegradable drug delivery composition is provided, which comprises: (a) a biodegradable triblock copolymer present in an amount of 3% to 45% (w %/w %) or 2% to 45% (w %/w %) or 1.2% to 30% (w %/w %) of the total composition having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer present in an amount of 8.0% to 50% (w %/w %) or 1% to 28% (w %/w %) of the total composition having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition and wherein the PEG in the diblock is end capped and (c) at least one pharmaceutically active principle is present in an amount of 1% to 20% (w %/w %) of the total composition or the at least one pharmaceutically active principle is present in an amount of 1 to 200 mg/ml.


In yet another aspect a biodegradable drug delivery composition is provided, which comprises: (a) a biodegradable triblock copolymer present in an amount of 3.0% to 45% (w %/w %) or 2% to 45% (w %/w %) or 1.2% to 30% (w %/w %) of the total composition having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer present in an amount of 8.0% to 50% (w %/w %) or 1% to 28% (w %/w %) of the total composition having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 in said biodegradable drug composition and wherein the PEG in the diblock is end capped and (c) at least one pharmaceutically hydrophobic active principle is present in an amount of 1% to 20% (w %/w %) of the total composition or the at least one pharmaceutically active principle is present in an amount of 1 to 200 mg/ml.


In yet another aspect a biodegradable drug delivery composition is provided, which comprises: (a) a biodegradable triblock copolymer present in an amount of 3.0% to 45% (w %/w %) or 2.0% to 45% (w %/w %) or 1.2% to 30% (w %/w %) of the total composition having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer present in an amount of 8.0% to 50% (w %/w %) or 1% to 28% (w %/w %) of the total composition having the formula:





PEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:3 to 1:8 or 3:2 to 1:19 or 1:1 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition and wherein the PEG in the diblock is end capped and (c) at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine. is present in an amount of 10% to 40% (w %/w %) or 1% to 40% (w %/w %) of the total composition or the at least one pharmaceutically active principle is present in an amount of 1 to 200 mg/ml or 0.1 to 200 mg/ml.


The biodegradable drug delivery compositions of the invention can have a lactic acid to ethylene oxide molar ratio in the composition of between 0.5 to 3.5 or from 0.5 to 2.5 or 0.5 to 22.3 for the triblock copolymer and between 2 to 6 or 0.8 to 13 for the diblock copolymer.


In another aspect the biodegradable drug delivery compositions of the invention can have a lactic acid to ethylene oxide molar ratio in the composition of between 0.5 to 22.3 for the triblock copolymer and between 0.8 to 13 for the diblock copolymer.


In yet another aspect the biodegradable drug delivery compositions of the invention can have a lactic acid to ethylene oxide molar ratio in the composition of between 0.5 to 2.5 for the triblock copolymer and between 3 to 5 for the diblock copolymer.


In one aspect the biodegradable drug delivery composition is an injectable liquid that when it is inserted into the body of an animal or plant becomes a hardened implant.


In yet another aspect the biodegradable delivery drug composition can be used as a spatial formulation such that it can be applied onto or inside the body of an animal or plant. For example, it can be dispensed during surgery to treat a wound or inside a plant to treat a virus.


In another aspect the biodegradable drug composition is prepared as small solid particles, which are placed directly on the injured site of the body of an animal or plant.


In another aspect the biodegradable drug composition is in the form of a rod implant.


A method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABU type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 (a):(b) to forma polymer mixture; and


(ii) adding at least one pharmaceutically active principle to said polymer mixture, is yet another aspect of the invention.


A method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to forma polymer mixture; and


(ii) adding at least one pharmaceutically active principle to said polymer mixture, is yet another aspect of the invention.


A method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to form a polymer mixture; and


(ii) adding at least one pharmaceutically hydrophobic active principle to said polymer mixture, is yet another aspect of the invention.


A method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to form a polymer mixture; and


(ii) adding at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture, is yet another aspect of the invention.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1060 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 in (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1060 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1060 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 (a):b) to form a polymer mixture; (ii) adding at least one pharmaceutically active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):b) to form a polymer mixture; (ii) adding at least one pharmaceutically active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect of the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090 or 4 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3.2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture; and (iii) evaporating said solvent.


In the above methods the organic solvent can be present in an amount of 40% to 74% (w %/w %) or 30% to 70% (w %/w %) or 26% to 90% (w %/w %) of the total composition. Mixtures of solvents can also be used.


Other aspects and embodiments are set forth below, or will readily arise from the following description of the preferred embodiments.





BRIEF DESCRIPTION OF THE DRAWINGS


FIG. 1 is a graph showing the in vitro release rate of the drug from formulations based on 40% P6R1(TB):dP2R4(DB) in ratios of 1:0 (-∘-), 1:2 (-Δ-), 1:4 (-●-), 1:6 (-▾-) and 1:9 (-*-) over time in days. This graph shows that formulations based on TB:DB are sustaining the release for more than 30 days.



FIG. 2 is a graph showing the in vitro cumulative percent release curve from candidate formulations of FIG. 1 over time (days). This graph illustrates that the initial burst is reduced and the drug release curve is flattened in the combination of triblock copolymer and diblock copolymer compositions compared to the triblock copolymer composition alone. It should be noted that the 1:9 curve is overlapping the 1:4 curve.



FIG. 3 is a graph showing the injectability of formulations based on 40% P6R1 (TB); dP2R4(DB) in various ratios ranging from 1:0 triblock copolymer to diblock copolymer to 0:1 triblock copolymer to diblock copolymer. This graph illustrates that all formulations are injectable using a classical injection device.



FIG. 4 is a graph showing the in vitro cumulative percentage release curve from candidate formulations over time (days) of various compositions of the invention. The compositions described as numbers 177, 246, 224, 225 and 250 are described in Table 1.



FIG. 5 is a graph showing the in vitro release rate from candidate formulations in micrograms per hour per gram of formulation (μg/h/gr of formulation) The compositions described as numbers 177, 246, 224, 225 and 250 are described in Table 1.



FIG. 6 is a graph showing the M53 plasma concentration in nanograms per milliliter (ng/ml) over time in days. Day zero is the day that the composition was administered subcutaneously. The compositions indicated as numbers 177, 246, 224, 225 and 250 are described in Table 1.



FIG. 7 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.2R5 (4 units of ethylene oxide and 24 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 8 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.2R14 (4 units of ethylene oxide and 58 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 9 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.2R22 (4 units of ethylene oxide and 89 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 10 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.4R4 (9 units of ethylene oxide and 41 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 11 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.4R7 (9 units of ethylene oxide and 67 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 12 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.6R1 (13 units of ethylene oxide and 26 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 13 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.6R3 (13 units of ethylene oxide and 40 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 14 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P0.6R4 (13 units of ethylene oxide and 55 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 15 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P1R2 (22 units of ethylene oxide and 47 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 16 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P1R3 (22 units of ethylene oxide and 68 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 17 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P1R4 (22 units of ethylene oxide and 88 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 18 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P2R2 (45 units of ethylene oxide and 88 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 19 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblockco polymer P2R3 (45 units of ethylene oxide and 157 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 20 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P2R5 (45 units of ethylene oxide and 216 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 21 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P3R1 (68 units of ethylene oxide and 66 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 22 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P3R2 (68 units of ethylene oxide and 154 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 23 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P3R3 (68 units of ethylene oxide and 218 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 24 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P6R0.9 (136 units of ethylene oxide and 125 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 25 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P6R1.6 (136 units of ethylene oxide and 218 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 26 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P6R2 (136 units of ethylene oxide and 272 units of lactic acid) mixed with various diblock copolymers (see Table 2 for details).



FIG. 27 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P2R4 (45 units of ethylene oxide and 157 units of lactic acid) mixed with diblock copolymer dP0.4R6 (7 units of ethylene oxide and 42 units of lactic acid) at different ratios (see Table 2 for details).



FIG. 28 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P2R4 (45 units of ethylene oxide and 157 units of lactic acid) mixed with diblock copolymer dP0.6R5 (12 units of ethylene oxide and 54 units of lactic acid) at different ratios (see Table 2 for details).



FIG. 29 is a graph showing the in vitro cumulative percent release of acetaminophen over time (days) from formulations based on triblock copolymer P2R5 (45 units of ethylene oxide and 216 units of lactic acid) mixed with diblock copolymer dP0.2R13 (3 units of ethylene oxide and 39 units of lactic acid) at different ratios (see Table 2 for details).



FIG. 30 is a graph showing the in vitro release rate of buprenorphine over time (days) from formulations no 33 (10% BN/8% P2R2/32% dP0.4R10), no 47 (10% BN/8% P2R2/32% dP1R3) and no 58 (10% BN/10% P0.4R8/40% dP1R2).



FIG. 31 is a graph showing the plasma concentration of buprenorphine over time (days) in rats injected with formulations no 33 (10% BN/8% P2R2/32% dP0.4R10), no 47 (10% BN/8% P2R2/32% dP1R3) and no 58 (10% BN/10% P0.4R8/40% dP1R2).



FIG. 32 is a graph showing the in vitro release rate of risperidone over time (days) from formulations based on triblock polymer P2R5 (45 units of ethylene oxide and 216 units of lactic acid) mixed with diblock polymer dP0.2R13 (3 units of ethylene oxide and 39 units of lactic acid) at different ratios (see Table 2 for details).



FIG. 33 is a graph showing the plasma concentration of risperidone and 9-OH risperidone over time (days) in rats injected with formulations no 10 (5% RSP/16% P2R2/24% dP2R2/DMSO), no 29 (10% RSP/24% P1R4/16% dP0.4R5/DMSO) and no 31 (10% RSP/18% P2R4/12% dP0.4R5/DMSO).



FIG. 34 is a graph showing the plasma concentration of ivermectin over time (days) in dogs injected with formulations no 7 (5% IVM/15% P3R3/25% dP0.4R5/DMSO), no 9 (5% IVM/15% P2R4/25% dP2R3/DMSO) and no 10 (5% IVM/15% P2R5/25% dP2R2/DMSO).



FIG. 35 is a graph showing the in vitro release rate of medroxyprogesterone acetate (MPA) from candidate formulations in milligrams per gram of formulation per day (mg MPA/gr of formulation/day) The formulations described as numbers 33, 34 and 49 as described in Table 6. In vitro release obtained with Depo-SubQ Provera is shown as a control.



FIG. 36 is a graph showing the in vitro cumulative percent release of medroxyprogesterone acetate over time (days) from formulations described 33, 34 and 49 as described in Table 6. In vitro release obtained with Depo-SubQ Provera is shown as a control.



FIG. 37 is a graph showing the in vitro release rate of medroxyprogesterone acetate from candidate formulations in milligrams per gram of formulation per day (mg/gr of formulation/day) The formulations described as numbers 12, 32 and 36 are described in Table 6. In vitro release obtained with Depo-SubQ Provera is shown as a control.



FIG. 38 is a graph showing the in vitro cumulative percent release of medroxyprogesterone acetate from formulations described 12, 32 and 36 per days are described in Table 6. In vitro release obtained with Depo-SubQ Provera is shown as a control.



FIG. 39 is a graph showing the plasma concentration of medroxyprogesterone acetate (MPA) in female dogs over time (days) injected with formulations 33, 34 and 49 described in Table 6. Each dog received a single 3 mg/kg dose of MPA.



FIG. 40 is a graph showing the plasma concentration of medroxyprogesterone acetate (MPA) in dogs over time (days) injected with formulations 12, 32 and 36 are described in Table 6. For formulations 32, 36 and the control group (receiving Depo-subQ-Provera), each dog received a single 3 mg/kg MPA dose. The group receiving formulation 12 was dosed at 6 mg/kg MPA.



FIG. 41 is a graph showing the in vitro percent total release of medroxyprogesterone acetate (MPA) over time (days) from formulations 7, 10 and 13 described in Table 6.



FIG. 42 is a graph showing the in vitro percent total release of medroxyprogesterone acetate (MPA) over time (days) from formulations 32 and 33 described in Table 6.



FIG. 43 is a graph showing the in vitro percent total release of medroxyprogesterone acetate (MPA) over time (days) from formulations 25, 27 and 30 described in Table 6.



FIG. 44 is a graph showing the in vitro percent total release of progesterone (Pro) over time (days) from formulations 11, 13 and 7 described in Table 7.



FIG. 45 is a graph showing the in vitro percent total release of progesterone (Pro) over time (days) from formulations 10, 12 and 5 described in Table 7.



FIG. 46 is a graph showing the in vitro percent total release of Levonorgestrel (Levo) over time (days) from formulations 7, 8 and 9 described in Table 8.



FIG. 47 is a graph showing the in vitro percent total release of Levonorgestrel (Levo) over time (days) from formulations 4, 5 and 6 described in Table 8.



FIG. 48
FIG. 42 is a graph showing the in vitro percent total release of cyclosporine (CSP) over time (days) from formulations 19, 20, 21, 22, 23 and 24 described in Table 9.



FIG. 49 is a graph showing the in vitro percent total release of Bupivacaine base (Bupi) over time (days) from formulations based on formulations 42, 47, 37, 35 and 34 described in Table 10.





DESCRIPTION OF THE PREFERRED EMBODIMENTS

As used herein the term “biodegradable” means that the triblock and diblock copolymers will after a period of time erode or degrade in vivo to form smaller non-toxic components.


The term “parenteral administration” encompasses intramuscular, intraperitoneal, intra-abdominal, subcutaneous, intravenous and intraarterial. It also encompasses intradermal, intracavernous, intravitreal, intracerebral, intrathecal, epidurall and intraosseous administration.


The term “animals” encompasses all members of the Kingdom Animalia.


As used herein the term “plant” encompasses all members of the Plant Kingdom.


“Active principle” means a drug or medicine for treating various medical illnesses. Thus active principles, drugs and medicines are used interchangeably. The term drug or active principle as used herein includes without limitation physiologically or pharmacologically active substances that act locally or systemically in the body of an animal or plant. At least one active principle is present in the biodegradable drug composition of the invention.


As used herein “disease” means any disorder in a human, animal or plant caused by infection, diet, or by faulty functioning of a process.


The term “implant” means that the drug delivery compositions are injectable, are in situ forming and are biodegradable and turn into solid implants when injected into the body. Thus, that the formulations that are synthesized are liquids such that they can be easily injected through a syringe without excessive force.


The term “spatial formulations” encompass any formulations that can be applied on or into the animal or plant body and do not necessarily have to be administered through a syringe.


As used herein “repeat units” are the fundamental recurring units of a polymer.


By “end-capped polyethylene glycol” (cPEG) refers to PEG's in which one terminal hydroxyl group is reacted and includes alkoxy-capped PEG's, urethane-capped PEG's ester-capped PEG's and like compounds. The capping group is a chemical group which does not contain a chemical function susceptible to react with cyclic esters like lactide, glycolactide, caprolactone and the like or other esters and mixtures thereof. The reaction of an end-capped PEG polymer with lactide generates a diblock cPEG-PLA copolymer.


As used herein polyethylene glycol, as abbreviated PEG throughout the application, is sometimes referred to as poly(ethylene oxide) or poly(oxyethylene) and the terms are used interchangeably in the present invention.


The abbreviation of “PLA” refers to poly(lactic acid).


The abbreviation of “PLGA” refers to poly(lactic-co-glycolic acid).


The abbreviation “T” or “TB” refers to a triblock copolymer(s), while the abbreviation “D” or “DB” refers to a diblock copolymer(s).


The term “diblock” as used herein refers, for example, to an end-capped PEG-polyester copolymer. “mPEG” refers to methoxy polyethylene glycol.


The term “triblock” refers, for example, to a polyester-PEG-polyester copolymer.


As used herein the term “partial suspension” means that the pharmaceutically active principle is in a partly soluble and partly solid form.


As used herein “hydrophobic” when referring to the pharmaceutically active principles means drugs that have poor solubility in aqueous solutions. The International Union of Pure and Applied Chemistry (IUPAC) defines solubility as “the analytical composition of a saturated solution expressed as a proportion of a designated solute in a designated solvent.” A substance is said to be soluble if more than 0.1 g of that substance dissolves in 100 ml of distilled water at 250° C. If less than 0.1 g dissolves in 100 ml of distilled water at 250° C. the substance is sparingly soluble or insoluble at a particular temperature.


The LA/EO ratio refers to the molar ratio of lactic acid units to ethylene oxide units that is present in the biodegradable drug delivery composition. It is determined experimentally by NMR. The LA/EO molar ratio of the combined triblock copolymer can range from 0.5 to 3.5. In another aspect the LA/EO molar ratio in the triblock can range from 0.5 to 2.5 in the biodegradable drug delivery composition described herein. In yet another aspect the LA/EO ratio in the triblock can range from 0.5 to 22.3.


The LA/EO ratio in the diblock can range from 2 to 6. In another aspect the LA/EO ratio in the diblock can range from 3 to 5 in the biodegradable drug delivery composition. In another aspect the LA/EO ratio in the diblock can range from 0.8 to 13.


The degree of polymerization or DP is the number of repeat units in an average polymer chain at time tin a polymerization reaction. For example, the degree of polymerization for PEG is about 45 to 170 or it can be 4 to 273 or 3 to 45 or 0.55 to 68, while for PLA it can range from about 84 to 327 or it can be 24 to 682 or 7 to 327 or 39.9 to 170.


The present invention thus relates to a biodegradable drug composition comprising a triblock copolymer and a diblock copolymer. The biodegradable triblock copolymer has the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging, for example, from 4 to 1090 or from 6 to 1090 and v=x or v≠x. w is the degree of polymerization (number of repeat units) for PEG. The degree of polymerization for DP-PEG is calculated by dividing the PEG molecular weight by the EO unit molecular weight (44 Da). v+x equals the degree of polymerization (number of repeat units) for PLA. DP-PLA is calculated by multiplying DP-PEG by the LA/EO ratio.


However the number of repeat units of v, w and x in the triblock composition may vary due to the targeted time of release of the active principle and the type of active principle itself. Therefore the number of repeat units in the triblock of v, w and x can range from 4 to 1090 or from 6 to 1090 or from 8 to 1090, from 10 to 850, from 20 to 700, from 30 to 650 and v=x or v≠x. For instance, w can be 273, while x+y can be 682 and v=x or v≠x or w can be 136 and x+y can be 273 and v=x or v≠x or w can be 45.5 and x+y can be 546 or w can be 273 and x+y can be 136.


The size of the PEG in the triblock can range from 194 Da to 12,000 Da.


The polyester in the triblock can be polylactic acid (PLA), polycaprolactone (PCL), polyglycolic acid (PGA) or polyhydroxyalkanoate (PHA). In one embodiment the polyester that is used is polylactic acid.


The triblock copolymer is then combined with a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or from 3 to 327 or 3 to 237. This combination has a ratio of triblock copolymer to diblock copolymer ranging from 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1.


Examples of end-capped polyethylene glycols include alkoxy capped PEG's such as methoxyPEG or ethoxyPEG, urethane-capped PEG's, ester-capped PEG's, amine-capped PEG's and amide-capped PEG's. This list of end-capped PEG's is not exhaustive and a person skilled in the art would recognize additional end-capped PEG's, which are not listed.


However the number of repeat units (degree of polymerization (DP)) of y and z in the diblock composition may also vary. Thus, y can, for example, range from 7 to 43 or 3 to 45 or 0.55 to 68 and z can range from 32 to 123 or 7 to 327 or 39.9 to 170. For example, y can be 25 and z can be 123, y can be 34.5 and z can be 123 or y can be 45 and z can be 32. The degree of polymerization for DP-PEG is calculated by dividing the PEG molecular weight of the capped PEG by the EO unit molecular weight (44 Da). The DP-PLA is calculated by multiplying DP-PEG by the LA/EO ratio.


The polyester in the diblock can be polylactic acid (PLA), polycaprolactone (PCL), polyglycolic acid (PGA), poly(lactic-co-glycolic acid) (PLGA) or polyhydroxyalkanoate (PHA). In one embodiment the polyester that is used is polylactic acid. In another embodiment the polyester is poly(lactic-co-glycolic acid).


In another aspect the present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x the number of are repeat units ranging from 4 to 1090 or from 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 in said biodegradable drug composition; and (c) at least one pharmaceutically active principle.


In another aspect the present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x the number of are repeat units ranging from 4 to 1090 or from 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle.


In another aspect the present invention provides a biodegradable drug delivery composition comprising (a) a biodegradable triblock copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x the number of are repeat units ranging from 4 to 1090 or from 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine.


In another aspect the present invention provides a biodegradable drug delivery composition comprising a biodegradable triblock copolymer having the formula: PLAv-PEGw-PLAx, wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; a biodegradable diblock copolymer having the formula: mPEGy-PLAz, wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 327, wherein the ratio of the biodegradable triblock copolymer and the biodegradable diblock copolymer is 1:6 in said biodegradable drug composition; and at least one pharmaceutically active principle.


In another aspect the present invention provides a biodegradable drug delivery composition comprising a biodegradable triblock copolymer having the formula: PLAv-PEGw-PLAx, wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; a biodegradable diblock copolymer having the formula: mPEGy-PLAz, wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 327, wherein the ratio of the biodegradable triblock copolymer and the biodegradable diblock copolymer is 1:6 in said biodegradable drug composition; and at least one pharmaceutically hydrophobic active principle.


In another aspect the present invention provides a biodegradable drug delivery composition comprising a biodegradable triblock copolymer having the formula: PLAv-PEGw-PLAx, wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; a biodegradable diblock copolymer having the formula: mPEGy-PLAz, wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 327, wherein the ratio of the biodegradable triblock copolymer and the biodegradable diblock copolymer is 1:6 or 2:3 or 3:2 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate levonorgestrel, cyclosporine, progesterone or bupivacaine.


In another aspect a biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





MPEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:4 in said biodegradable drug composition; and (c) at least one pharmaceutically active principle.


In another aspect a biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





MPEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:4 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle.


In another aspect a biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula:





PLAv-PEGw-PLAx


wherein v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x; (b) a biodegradable diblock copolymer having the formula:





mPEGy-PLAz


wherein y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, wherein the ratio of the biodegradable triblock copolymer of (a) and the biodegradable diblock copolymer of (b) is 1:4 or 2:3 or 3:2 or 4:1 or 2.3 to 4.1 in said biodegradable drug composition; and (c) at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine.


The ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 in said biodegradable drug composition. In one embodiment the ratio of the biodegradable triblock copolymer of and the biodegradable CA diblock copolymer is selected from the group of 1:3, 1:4, 1:5, 1:6, 1:7 and 1:8 or 1:1, 1:2, 1:3, 1:4, 1:5, 1:6, 1:7, 1:8, 1:9, 1:10, 1:11, 1:12, 1:13, 1:14, 1:15, 1:16, 1:17, 1:18 and 1:19. It can also be 3:2 or 2:3 or 4:1. In another aspect the ratio of the triblock to the diblock is 1:6.


The length of the polyester chain is defined by its polyester to ethylene oxide molar ratio, which is between 0.5 to 3.5 or 0.5 to 2.5 or 0.5 to 22.3 for the triblock copolymer and 3 to 5 or 2 to 6 or 0.8 to 13 for the diblock copolymer. Thus, for example, if polylactic acid is used the chain length is defined by the lactic acid/ethylene oxide molar ratio. Similarly if polyglycolic acid is used, the chain length is defined by the polyglycolic acid/ethylene oxide molar ratio or the polycaprolactone/ethylene oxide molar ratio or the polyhydroxyalkanoate/ethylene oxide molar ratio. If poly(lactic-co-glycolic) acid is used the chain length is defined by the ratio of LA+G/EO.


The mass of the end-capped polyethylene glycol can range from 164 Da to 2,000 Da or from 100 Da to 2 kDa. It can range in the lower 100 to 300 Da range or in the 1 kDa to 2 kDa range.


The size of the polyethylene glycol chain ranges from 200 Da to 12 kDa in the biodegradable drug delivery composition or it can range from 400 Da to 12 kDa or 194 Da to 12 kDA.


The polymers are present in an amount of 20% to 50% (w %/w %) of the total weight of the composition. In another aspect the total weight of the polymers present in the biodegradable drug composition is 30% to 50% (w %/w %) of the total weight of the composition. In yet another aspect the polymers are present in the biodegradable drug composition at 40% to 50% (w %/w %) of the total weight of the composition. In another aspect the polymers are present in an amount of 5% to 40% (w %/w %) of the total composition or 5% to 50% (w %/w %) of the total composition. In yet another aspect the polymers are present in the biodegradable drug composition at 2.5% to 40% (w %/w %) or 2.5% to 50% (w %/w %) of the total weight of the composition.


Thus, the triblock copolymer is present in an amount of 3.0% to 45% (w %/w %) of the total weight of the composition. In another aspect the triblock copolymer is present in an amount of 6% to 10% (w %/w %) of the total weight of the composition. In yet another aspect the triblock copolymer is present in an amount of 20% to 40% (w %/w %) of the total weight of the composition. In yet another aspect the triblock copolymer is present in an amount of 1.2% to 30% (w %/w %) of the total weight of the composition or 1.2% to 45% (w %/w %) of the total weight of the composition.


In another embodiment the triblock copolymer is present in 3.3% to 4.0% (w %/w %) or 3.5% (w %) or 4.0% (w %) or 1.9% to 4.0% (w %/w %) of the total weight of the composition.


Likewise the diblock copolymer can be present in the biodegradable drug composition in an amount of 8% to 50% (w %/w %) of the total weight of the composition. In another aspect the diblock copolymer is present in an amount of 10% to 20% (w %/w %) of the total weight of the composition. In yet another aspect the diblock copolymer is present in an amount of 20% to 40% (w %/w %) of the total weight of the composition. In yet another aspect the diblock copolymer is present in an amount of 1% to 28% (w %/w %) of the total weight of the composition or 1% to 50% (w %/w %) of the total weight of composition.


In yet another embodiment the diblock is present in an amount of 2.48% to 5.02% (w %/w %) or 2.3% to 5.4% (w %/w %) or 2.5% to 5.1% (w %/w %) or 2.3% (w %) or 2.3% to 5.8% (w %/w %) of the total weight of the composition.


The at least one pharmaceutically active principle is entrapped in the triblock: diblock biodegradable drug delivery composition. Representative drugs and biologically active agents to be used in the invention include, without limitation, peptide drugs, protein drugs, desensitizing agents, antigens, vaccines, vaccine antigens, anti-infectives, antibiotics, antimicrobials, antiallergenics, anti-diabetics, steroidal anti-inflammatory agents, decongestants, miotics, anticholinergics, sympathomimetics, sedatives, hypnotics, psychic energizers, tranquilizers, androgenic steroids, estrogens, progestational agents, medroxyprogesterone acetate, humoral agents, prostaglandins, analgesics, corticosteroids, antispasmodics, antimalarials, antihistamines, cardioactive agents, non-steroidal anti-inflammatory agents, antiparkinsonian agents, antihypertensive agents, beta-adrenergic blocking agents, nutritional agents, gonadotrophin releasing hormone agonists, insecticides, anti-helminthic agents and the benzophenanthridine alkaloids.


Thus combinations of drugs can also be used in the biodegradable drug delivery composition of this invention. For instance, if one needs to treat Lupus erythematosis, non-steroidal anti-inflammatory agents and corticosteroids can be administered together in the present invention.


In an embodiment the pharmaceutically active principle is a hydrophobic drug having a low solubility or is insoluble in aqueous solutions. Hydrophpbioc drugs are described herein and include, for example, amphotericin, anthralin, beclomethasone, betamethasone, camptothecin, curcum in, dexamethasone, genistein, indomethacin, lidocaine, taxol, tetracycline, tretinoin, therapeutic proteins that are insoluble in water and the like. In one embodiment the pharmaceutically active principle is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine.


Veterinary medicaments such as medicines for the treatment of worms or vaccines for animals are also part of the present invention. Hydrophobic veterinary drugs can also be formulated in the biodegradable drug compositions as described herein.


Viral medicaments for plants such as those viruses from Potyviridae, Geminiviridae, the Tospovirus genus of Bunyaviridiae and Banana streak virus are also encompassed by the present invention. Also medicaments for tobacco mosaic virus, turnip crinkle, barley yellow dwarf, ring spot watermelon and cucumber mosaic virus can be used in the biodegradable drug delivery composition of the invention. Hydrophobic viral medicaments for plants can also be formulated in the biodegradable drug compositions as described herein.


To those skilled in the art, other drugs or biologically active agents that can be released in an aqueous environment can be utilized in the described delivery system. Also, various forms of the drugs or biologically active agents may be used. These include without limitation forms such as uncharged molecules, molecular complexes, salts, ethers, esters, amides, etc., which are biologically activated when injected into the animal or plant or used as a spatial formulation such that it can be applied on or inside the body of an animal or plant or as a rod implant.


The pharmaceutically effective amount of an active principle or hydrophobic active principle may vary depending on the active principle, the extent of the animal's or plants medical condition and the time required to deliver the active principle or hydrophobic active principle. There is no critical upper limit on the amount of active principle or hydrophobic active principle incorporated into the polymer solution except for that of an acceptable solution or dispersion viscosity for injection through a syringe needle and that it can effectively treat the medical condition without subjecting the animal or plant to an overdose. The lower limit of the active principle or hydrophobic active principle incorporated into the delivery system is dependent simply upon the activity of the active principle or hydrophobic active principle and the length of time needed for treatment.


For instance some active principles or hydrophobic active principles may be present in the biodegradable drug delivery composition from 10 to 200 mg/ml. In another aspect the drugs should be present in the amount of 10 to 40 μg/ml. In another aspect the drugs should be present in the amount of 10 to 500 mg/ml. For a small molecule, for instance, the active principle can be loaded as high as 100 to 200 mg per ml.


Generally the pharmaceutically active principle is present in an amount of 1% to 20% (w %/w %) of the total weight of the composition. In another aspect the active principle is present in 1% to 4% (w %/w %) of the total weight of the composition. In another aspect the active principle is present in 2% to 4% (w %/w %) of the total weight of the composition. In yet another aspect the active principle, which is a small molecule, is present in an amount of 10% to 20% (w %/w %) of the total weight of the composition. In another aspect the active principle is present in an amount of 10% to 40% (w %/w %) of the total composition. In another embodiment the pharmaceutically active hydrophobic active principle is present in the amounts of 1% to 40% (w %/w %).


As examples, the medroxyprogesterone acetate can be present in an amount of 10% to 40% (w %/w %) of the total weight of the biodegradable drug delivery compositions; the progesterone can be present in an amount of 20% to 40% (w %/w %) of the total weight of the biodegradable drug delivery compositions; the cyclosporine can be present in an amount of 5% to 21.1% (w %/w %) of the total weight of the biodegradable drug delivery compositions; levonorgestrel can be present in an amount of 10% to 20% (w %/w %) of the total weight of the biodegradable drug delivery compositions; and the bupivacaine can be present in an amount of 1% to 15% (w %/w %) of the total weight of the biodegradable drug delivery compositions.


In the biodegradable drug delivery composition of the present invention, the pharmaceutically effective amount can be released gradually over an extended period of time. This slow release can be continuous or discontinuous, linear or non-linear and can vary due to the composition of the triblock copolymer and diblock copolymer. Thus, the higher the lactic acid content of the triblock and diblock copolymers in comparison with the polyethylene glycol content, as well as the amount of triblock and diblock copolymers present in the biodegradable drug composition the longer the release of the active principle or hydrophobic active principle or drug. In other words, the higher the LA/EO molar ratio and the greater weight percentage of the triblock and diblock copolymers, the longer it will take for the active principle or hydrophobic active principle to be released from the drug composition.


The active principle or hydrophobic active principle can be released for a duration of between 7 days to 1 year or longer depending upon the type of treatment needed and the biodegradable drug delivery composition used. In one aspect the biodegradable drug delivery composition can deliver the active principle or hydrophobic active principle for at least 7 days. In another aspect the biodegradable drug delivery composition can deliver the active principle or hydrophobic active principle for at least 30 days. In one aspect the biodegradable drug delivery composition can deliver the active principle or hydrophobic active principle for at least 90 days. In yet another aspect the biodegradable drug delivery composition can deliver an active principle or hydrophobic active principle for 1 year or longer.


The biodegradable drug delivery composition can be an injectable liquid or a partial suspension at room temperature and be injected through a syringe without excessive force. But these biodegradable drug delivery compositions are also in situ forming and biodegradable and turn into solid implants when injected into the animal or plant. Alternatively the biodegradable drug composition is produced as a solid, prepared as small particles and used as a powder which is sprinkled on the injured site. In another aspect the drug delivery composition is a rod implant, which can be implanted under the skin or in another compartment in the body. In another aspect the drug delivery composition can be prepared and applied as a film. In yet another aspect the biodegradable delivery drug composition can be used as a spatial formulation such that it can be applied onto or inside the body of an animal or plant. It can be applied anywhere on the body, including in the eye. In another aspect the biodegradable drug composition can be produced as a partial suspension, the drug being in between the state of being partly soluble and partly solid.


The biodegradable drug delivery composition can further comprise a pharmaceutically acceptable carrier, adjuvant or vehicle. An acceptable carrier can be saline, buffered saline and the like. It can be added to the biodegradable drug delivery composition after its formulation with the drug and diblock copolymer and triblock copolymer.


The adjuvant can be formulated simultaneously when mixing the drug. In this regard the adjuvants that can be used are alum, aluminum phosphate, calcium phosphate, MPL™, CpG motifs, modified toxins, saponins, endogenous stimulatory adjuvants such as cytokines, Freunds complete and incomplete adjuvants, ISCOM type adjuvants, muramyl peptides and the like.


The vehicle can be any diluent, additional solvent, filler or binder that may alter the delivery of the active principle when needed in the biodegradable drug delivery composition. Examples include small amounts of triglycerides such as triacetin or tripropionin. The amount that can be used in the present biodegradable drug deliver compositions of the present invention can vary from 12% to 20% (w %/w %). In one aspect a triacetin can be added in the formulation at 17.0% (w %/w %). In another aspect tripropionin (abbreviated herein as Tripro) can be added at 16% (w %/w %). In yet another aspect benzyl alcohol can be added at 15% to 35% (w %/w %).


A method for preparing the biodegradable drug delivery composition of the invention is also encompassed by the invention. This method comprises: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090; and (b) a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237 in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 triblock to diblock to form a polymer mixture; and adding at least one pharmaceutically active principle to said polymer mixture.


A method for preparing the biodegradable drug delivery composition of the invention is also encompassed by the invention. This method comprises: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090; and (b) a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237 in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 triblock to diblock to form a polymer mixture; and adding at least one pharmaceutically hydrophobic active principle to said polymer mixture.


A method for preparing the biodegradable drug delivery composition of the invention is also encompassed by the invention. This method comprises: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax,


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az,


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237 in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 triblock to diblock to form a polymer mixture; and adding at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture.


A method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 (a):(b) to form a polymer mixture; and (ii) adding at least one pharmaceutically active principle to said polymer mixture, is yet another aspect of the invention.


A method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to form a polymer mixture; and


(ii) adding at least one pharmaceutically hydrophobic active principle to said polymer mixture, is yet another aspect of the invention.


A method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to form a polymer mixture; and


(ii) adding at least one pharmaceutically active principle one of which is medroxyprogesterone acetate, levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture, is yet another aspect of the invention.


Yet another aspect the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 137 in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 137 in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 137 in a ratio of 1:3 to 1:8 or 1:1 to 1:19 or 3:2 to 1:19 or 2:3 or 4:1 or 2.3 to 4.1 (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:4 (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:4 (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle to said polymer mixture; and (iii) evaporating said solvent.


Yet another aspect the present invention provides a method for preparing the biodegradable drug delivery composition of the present invention said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula:





Av-Bw-Ax


wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 6 to 1090, v and x being ester repeat units and w being ethylene oxide repeat units wherein v=x or v≠x; and (b) a biodegradable diblock copolymer having the formula:





Cy-Az


wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237, y being the number of ethylene oxide repeat units and z the number of ester repeat units, in a ratio of 1:4 or 2:3 or 3:2 or 4:1 (a):(b) to form a polymer mixture; (ii) adding at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture; and (iii) evaporating said solvent.


Another embodiment provides a method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090; and (b) a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237 in a ratio of 1:6 triblock to diblock to form a polymer mixture; adding at least one pharmaceutically active principle to said polymer mixture; and evaporating said solvent. In this aspect no solvent is present in the biodegradable drug delivery composition.


Another embodiment provides a method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090; and (b) a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237 in a ratio of 1:6 triblock to diblock to form a polymer mixture; adding at least one pharmaceutically hydrophobic active principle to said polymer mixture; and evaporating said solvent. In this aspect no solvent is present in the biodegradable drug delivery composition.


Another embodiment provides a method for preparing the biodegradable drug delivery composition of the invention, said method comprising: (i) dissolving in an organic solvent (a) a biodegradable ABA type block copolymer having the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090; and (b) a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237 in a ratio of 1:6 or 2:3 or 3:2 or 4:1 or 2.3 to 4.1 triblock to diblock to form a polymer mixture; adding at least one pharmaceutically hydrophobic active principle one of which is medroxyprogesterone acetate levonorgestrel, cyclosporine, progesterone or bupivacaine to said polymer mixture; and evaporating said solvent. In this aspect no solvent is present in the biodegradable drug delivery composition.


The organic solvent that can be used in the method described herein is selected from the group of: benzyl alcohol, benzyl benzoate, diethylene glycol dimethyl ether (Diglyme), diethylene glycol monoethyl ether (DEGMEE), dimethyl isosorbide (DMI), dimethyl sulfoxide (DMSO), ethyl acetate, ethyl benzoate, ethyl lactate, ethylene glycol monoethyl ether acetate, glycerol formal, methyl ethyl ketone, methyl isobutyl ketone, N-ethyl-2-pyrrolidone, N-methyl-2-pyrrolidone (NMP), pyrrolidone-2, tetraglycol, triacetin, tributyrin, tripropionin (tripro), or triethylene glycol dimethyl ether (triglyme) and mixtures thereof.


The organic solvent is present in an amount of 40% to 74% (w %/w %) of the total composition. In another aspect the organic solvent used in the preparation of the biodegradable drug delivery composition is present in an amount of 50% to 60% (w %/w %) of the total composition. In yet another aspect the solvent used in the preparation of the biodegradable drug delivery composition is present in an amount of 60% to 70% (w %/w %) of the total composition. In yet another aspect, the solvent used in the preparation of the biodegradable drug delivery system is present in the amount of 30%% to 70% (w %/w %) of the total composition. In another embodiment the organic solvent is present in the amount of 30% to 90% (w %/w %) of the total composition.


As examples, when medroxyprogesterone acetate is the active principle 30% to 70% (w %/w %) of the total composition of solvent is used; when progesterone is the active principle 40% to 80% (w %/w %) of the total composition of solvent is used; when cyclosporine is the active principle 55% to 72.9% (w %/w %) of the total composition of solvent is used; when levonorestrel is the active principle 70% to 90% (w %/w %) of the total composition of solvent is used; and when bupivacaine base is the active principle 62.5% to 80% (w %/w %) of the total composition of solvent is used.


Some mPEG-OH are contaminated with a small amount of OH-PEG-OH. By following the methods of the present invention and using the contaminated mPEG-OH the final product would be mPEG-PLA contaminated with a small amount of PLA-PEG-PLA, which is encompassed by the present invention. This contamination is less than 2%.


Another aspect of the present invention is the use of diblock and triblock copolymers for the manufacture of a biodegradable drug composition. In this respect the biodegradable triblock copolymer has the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x. The polyester can be polylactic acid (PLA), polycaprolactone (PCL), polyglycolic acid (PGA) or polyhydroxyalkanoate (PHA). In one embodiment the polyester that is used is poly (lactic) acid.


The triblock copolymer is then combined with a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237. The polyester can be polylactic acid (PLA), polycaprolactone (PCL), polyglycolic acid (PGA), poly (lactic-co-glycolic acid (PLGA) or polyhydroxyalkanoate (PHA). In one embodiment the polyester that is used is poly (lactic) acid.


The pharmaceutically active principle is then combined with the triblock and diblock


In yet another aspect of the present invention is the use of diblock and triblock copolymers for the manufacture of a biodegradable drug composition. In this respect the biodegradable triblock copolymer has the formula: Av-Bw-Ax, wherein A is a polyester and B is polyethylene glycol and v, w and x are the number of repeat units ranging from 4 to 1090 or 6 to 1090 and v=x or v≠x. The polyester can be polylactic acid (PLA), polycaprolactone (PCL), polyglycolic acid (PGA) or polyhydroxyalkanoate (PHA). In one embodiment the polyester that is used is poly (lactic) acid.


The triblock copolymer is then combined with a biodegradable diblock copolymer having the formula: Cy-Az, wherein A is a polyester and C is an end-capped polyethylene glycol and y and z are the number of repeat units ranging from 7 to 371 or 3 to 237. The polyester can be polylactic acid (PLA), polycaprolactone (PCL), polyglycolic acid (PGA), poly (lactic-co-glycolic acid (PLGA) or polyhydroxyalkanoate (PHA). In one embodiment the polyester that is used is poly (lactic) acid.


The pharmaceutically hydrophobic active principle is then combined with the triblock and diblock and can be medroxyprogesterone acetate levonorgestrel, cyclosporine, progesterone or bupivacaine base.


The ratio of the biodegradable triblock copolymer of (a) and the biodegradable CA diblock copolymer of (b) is 1:3 to 1:8 in said biodegradable drug composition. In one embodiment the ratio of the biodegradable triblock copolymer of and the biodegradable CA diblock copolymer is selected from the group of 1:3, 1:4, 1:5, 1:6, 1:7 and 1:8. or 1:1, 1:2, 1:3, 1:4, 1:5, 1:6, 1:7, 1:8, 1:9, 1:10, 1:11, 1:12, 1:13, 1:14, 1:15, 1:16, 1:17, 1:18 and 1:19. In another aspect the ratio of the triblock to the diblock is 1:6. It can also be 3:2 or 2:3 or 4:1 or 2.3 to 4.1.


The length of the polyester chain is defined by its polyester to ethylene oxide molar ratio, which is between 0.5 to 3.5 or 0.5 to 2.5 or 0.5 to 22.3 for the triblock and 3 to 5 or 2 to 6 or 0.8 to 13 for the diblock.


The mass of the end-capped polyethylene glycol can range from 100 Da to 2 kDa or 164 Da to 2 kDa. It can range in the 100 to 300 Da range or in the 1 kDa to 2 kDa range.


The size of the polyethylene glycol chain ranges from 200 Da to 12 kDa in the biodegradable drug delivery composition or it can range from 400 Da to 12 kDa or 194 Da to 12 kDa.


A number of embodiments and/or aspects of the invention have been described. Nevertheless it will be understood that various modifications may be made without departing from the spirit and scope of the invention.


EXAMPLES
Example 1—Polymer Synthesis

Copolymers were synthesized according to the method described in the U.S. Pat. No. 6,350,812, incorporated herein by reference, with minor modifications. Typically, the necessary amount of PEG (gives the triblock coploymer) or methoxy-PEG (gives the diblock copolymer) was heated at 65° C. and dried under vacuum for 2 hours in a reactor vessel. DL-lactide (corresponding to the targeted LA/EO molar ratio) and zinc lactate (1/1000 of amount of lactide) were added. The reaction mixture was first dehydrated by three short vaccum/N2 cycles. The reaction mixture was heated at 140° C. and rapidly degassed under vacuum. The reaction was conducted for four days at 140° C. under constant nitrogen flow (0.2 bar). The reaction was cooled to room temperature and its content was dissolved in acetone and then subjected to precipitation with ethanol. The product obtained was subsequently dried under reduced pressure. The final product was characterized by 1H NMR for its lactate content. The triblock PLA-PEG-PLA polymers described herein were labeled PxRy where x represent the size of the PEG chain in kDa and y is the LA/EO molar ratio. The diblock mPEG-PLA polymers described herein were labeled dPxRy where x represent the size of the PEG chain in kDa and y is the LA/EO molar ratio.


Example 2—Formulation Preparation Specific for the Peptide M53

The formulations described herein were based on organic solution of polymers containing as the drug, the peptide M53, a GLP-1 analogue. Typically, 0.4 grams of polymers, corresponding to a mix of a diblock copolymer and a triblock copolymer in defined mass ratio, were dissolved in 0.57 grams of a biocompatible solvent at room temperature overnight under constant magnetic stirring. The solvent was either a single solvent or a combination of solvents. The next day, 20 mg of drug was added to the polymer solution and stirred until complete dissolution. When the drug was not soluble in the solvent, a suspension of the drug in a polymer solution was obtained. Alternatively, the drug was dissolved or suspended in the biocompatible solvent and the polymer(s) added subsequently. The formulations were loaded in a syringe before use.


Example 3—the Formulations that were Prepared

Following Examples 1 and 2 various formulations were prepared, which are set forth in Table 1 for the peptide M53













TABLE 1









Triblock copolymer (TB)
Diblock copolymer (DB)

















M53

PEG

PEG

Solvent 1
Solvent 2


























Ratio
%
%

size
Ratio
DP-
DP-
%

size
Ratio
DP-
DP-

%

%

























No
DB/TB
(w/w)
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
Name
(w/w)
Name
(w/w)




























10
4.0
4.0
10.0%
P12R0.5
12
0.5
273
136
40.0%
dP2R3
2
3.2
45
143
DEGMEE
46.0%




12
4.0
4.0
10.0%
P12R3
12
2.5
273
682
40.0%
dP2R3
2
3.2
45
143
DEGMEE
46.0%


21
4.0
4.0
10.0%
P12R0.5
12
0.5
273
136
40.0%
dP2R3
2
3.2
45
143
Diglyme
46.0%


23
4.0
4.0
10.0%
P12R3
12
2.5
273
682
40.0%
dP2R3
2
3.2
45
143
Diglyme
46.0%


34
4.0
4.0
10.0%
P12R0.5
12
0.5
273
136
40.0%
dP2R3
2
3.2
45
143
DMI
46.0%


45
4.0
4.0
10.0%
P12R3
12
2.5
273
682
40.0%
dP2R3
2
3.2
45
143
DMI
46.0%


66
4.0
4.0
10.0%
P12R0.5
12
0.5
273
136
40.0%
dP2R3
2
3.2
45
143
Diglyme
46.0%


68
4.0
4.0
10.0%
P12R3
12
2.5
273
682
40.0%
dP2R3
2
3.2
45
143
Diglyme
46.0%


76
4.0
4.0
10.0%
P12R0.5
12
0.5
273
136
40.0%
dP2R3
2
3.2
45
143
DMSO
46.0%


78
4.0
4.0
10.0%
P12R3
12
2.5
273
682
40.0%
dP2R3
2
3.2
45
143
DMSO
46.0%


80
4.0
4.0
10.0%
P12R0.5
12
0.5
273
136
40.0%
dP2R3
2
3.2
45
143
Et Lactate
46.0%


82
4.0
4.0
10.0%
P12R3
12
2.5
273
682
40.0%
dP2R3
2
3.2
45
143
Et Lactate
46.0%


105
4.0
4.0
8.0%
P6R0.9
6
0.9
136
123
32.0%
dP2R4
2
4.4
45
200
Diglyme
56.0%


116
4.0
4.0
8.0%
P6R0.9
6
0.9
136
123
32.0%
dP2R4
2
4.4
45
200
Diglyme
56.0%


123
4.0
4.0
8.0%
P3R1
3
1.0
68
68
32.0%
dP2R4
2
4.3
45
195
DMSO
56.0%


124
4.0
4.0
8.0%
P6R0.9
6
0.9
136
123
32.0%
dP2R4
2
4.3
45
195
DMSO
56.0%


153
4.0
4.0
7.0%
P12R0.5
12
0.5
273
136
28.0%
dP2R4
2
4.3
45
195
DMSO
61.0%


159
4.0
4.0
7.0%
P12R0.5
12
0.5
273
136
28.0%
dP2R4
2
4.3
45
195
DMSO
44.0%
Tracetin
17.0%


169
5.7
2.0
6.0%
P6R0.9
6
0.9
136
123
34.0%
dP2R4
2
4.3
45
195
DMSO
58.0%


177
5.7
2.0
7.5%
P6R0.9
6
0.9
136
123
42.5%
dP2R4
2
4.3
45
195
DMSO
48.0%


198
9.0
4.0
4.0%
P6R0.9
6
0.9
136
123
36.0%
dP2R4
2
4.3
45
195
Diglyme
37.0%
Tripro
19.0%


200
9.0
2.0
5.0%
P6R0.9
6
0.9
136
123
45.0%
dP2R3
2
3
45
136
DMSO
48.0%


203
4.0
2.0
10.0%
P6R0.9
6
0.9
136
123
40.0%
dP2R7
2
7.2
45
327
DMSO
48.0%


207
5.7
4.0
6.0%
P6R0.9
6
0.9
136
123
34.0%
dP2R4
2
4.3
45
195
Diglyme
40.0%
Tripro
16.0%


209
4.0
2.0
9.0%
P6R0.9
6
0.9
136
123
36.0%
dP2R7
2
7.2
45
327
DMSO
53.0%


210
4.0
2.0
8.0%
P6R0.9
6
0.9
136
123
32.0%
dP2R7
2
7.2
45
327
DMSO
58.0%


221
9.0
4.0
5.0%
P6R0.9
6
0.9
136
123
45.0%
dP2R4
2
4.3
45
195
Diglyme
33.0%
Tripro
13.0%


224
5.7
2.0
6.0%
P6R0.9
6
0.9
136
123
34.0%
dP2R4
2
4.3
45
195
Diglyme
41.4%
Tripro
16.6%


225
9.0
2.0
5.0%
P6R0.9
6
0.9
136
123
45.0%
dP2R4
2
4.3
45
195
Diglyme
34.0%
Tripro
13.6%


230
5.7
2.0
7.5%
P6R0.9
6
0.9
136
123
42.5%
dP1R5
1
5.4
23
123
DMSO
48.0%


234
5.7
2.0
6.0%
P6R0.9
6
0.9
136
123
34.0%
dP1R5
1
5.4
23
123
Diglyme
41.4%
Tripro
16.6%


241
5.9
2.0
6.5%
P6R0.9
6
0.9
136
123
38.5%
dP1R5
1
5.4
23
123
DMSO
53.0%


245
5.9
2.0
6.5%
P2R2
2
2
45
91
38.5%
dP1R5
1
5.4
23
123
DMSO

53%



246
5.7
2.0
7.5%
P2R2
2
2
45
91
42.5%
dP1R5
1
5.4
23
123
DMSO
48.0%


247
9.0
2.0
5.0%
P2R2
2
2
45
91
45.0%
dP1R5
1
5.4
23
123
DMSO
48.0%


250
9.0
4.0
5.0%
P6R0.9
6
0.9
136
123
45.0%
dP2R4
2
4.3
45
195
Diglyme
33.2%
Tripro
12.8%









Example 4—Acetaminophen's Formulations Preparation

The formulations described herein were based on organic solution of polymers prepared as in Example 1, containing as the drug, acetaminophen. Typically, 0.4 grams of polymers, corresponding to a mix of a diblock copolymer and a triblock copolymer in defined mass ratio, were dissolved in 0.55 grams of dimethyl sulfoxide at room temperature overnight under constant magnetic stirring. The next day, 50 mg of acetaminophen was added to the polymer solution and stirred until complete dissolution. The formulations were loaded in a syringe before use. The composition of the various formulations is shown in Table 2 below, where the solvent used is DMSO.



FIGS. 7 to 26 illustrate the results of these formulations which show all possible combinations of 15 triblock copolymers with 20 diblocks copolymers.













TABLE 2









Triblock copolymer (TB)
Diblock copolymer (DB)
Solvent






















Exp
Ratio
%

PEG
Ratio
DP-
DP-
%

PEG
Ratio
DP-
DP-

%


no
DB/TB
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
Name
(w/w)

























1
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


2
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


3
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


4
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


5
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


6
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


7
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


8
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


9
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


10
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


11
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


12
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


13
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


14
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


15
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


16
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


17
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


18
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


19
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


20
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


21
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


22
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


23
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


24
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


25
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


26
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


27
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


28
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


29
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


30
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


31
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


32
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


33
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


34
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


35
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


36
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


37
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


38
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


39
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


40
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


41
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


42
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


43
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


44
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


45
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


46
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


47
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


48
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


49
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


50
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


51
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


52
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


53
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


54
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


55
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


56
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


57
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


58
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


59
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


60
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


61
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


62
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


63
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


64
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


65
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


66
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


67
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


68
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


69
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


70
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


71
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


72
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


73
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


74
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


75
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


76
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


77
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


78
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


79
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


80
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


81
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


82
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


83
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


84
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


85
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


86
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


87
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


88
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


89
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


90
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


91
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


92
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


93
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


94
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


95
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


96
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


97
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


98
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


99
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


100
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


101
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


102
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


103
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


104
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


105
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


106
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


107
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


108
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


109
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


110
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


111
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


112
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


113
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


114
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


115
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


116
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


117
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


118
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


119
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


120
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


121
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


122
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


123
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


124
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


125
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


126
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


127
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


128
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


129
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


130
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


131
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


132
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


133
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


134
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


135
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


136
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


137
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


138
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


139
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


140
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


141
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


142
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


143
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


144
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


145
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


146
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


147
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


148
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


149
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


150
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


151
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


152
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


153
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


154
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


155
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


156
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


157
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


158
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


159
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


160
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


161
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


162
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


163
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


164
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


165
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


166
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


167
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


168
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


169
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


170
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


171
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


172
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


173
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


174
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


175
4.0
8%
P0.2R6
0.2
5.9
4
24
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


176
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


177
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


178
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


179
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


180
4.0
8%
P0.2R22
0.2
22.3
4
89
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


181
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


182
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


183
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


184
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


185
4.0
8%
P0.4R5
0.4
4.7
9
41
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


186
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


187
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


188
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


189
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


190
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


191
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


192
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


193
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


194
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


195
4.0
8%
P0.6R2
0.6
1.9
13
26
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


196
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


197
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


198
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


199
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


200
4.0
8%
P0.6R4
0.6
4.2
13
55
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


201
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


202
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


203
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


204
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


205
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


206
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


207
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


208
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


209
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


210
4.0
8%
P1R4
1.0
4.0
22
88
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


211
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


212
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


213
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


214
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


215
4.0
8%
P2R2
2.0
2.0
45
88
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


216
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


217
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


218
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


219
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


220
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


221
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


222
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


223
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


224
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


225
4.0
8%
P3R1
3.0
1.0
68
66
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


226
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


227
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


228
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


229
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


230
4.0
8%
P3R3
3.0
3.2
68
218
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


231
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


232
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


233
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


234
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


235
4.0
8%
P6R0.9
6.0
0.9
136
125
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


236
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.2R6
0.2
5.8
3
17
DMSO
55%


237
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


238
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


239
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP1R4
1.0
4.0
22
89
DMSO
55%


240
4.0
8%
P6R2
6.0
2.0
136
272
32%
dP2R3
2.0
2.8
45
125
DMSO
55%


241
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


242
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


243
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


244
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


245
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


246
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


247
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


248
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


249
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


250
4.0
8%
P0.2R14
0.2
14.5
4
58
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


251
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


252
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


253
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


254
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


255
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


256
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


257
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


258
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


259
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


260
4.0
8%
P0.6R3
0.6
3.0
13
40
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


261
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


262
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


263
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


264
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


265
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


266
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


267
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


268
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


269
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


270
4.0
8%
P1R3
1.0
3.1
22
68
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


271
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


272
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


273
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


274
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


275
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


276
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


277
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


278
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


279
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


280
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


281
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


282
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


283
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


284
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


285
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


286
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


287
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


288
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


289
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


290
4.0
8%
P3R2
3.0
2.3
68
154
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


291
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.2R2
0.2
2.2
3
7
DMSO
55%


292
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


293
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.4R2
0.4
2.0
7
14
DMSO
55%


294
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


295
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.6R3
0.6
3.0
12
35
DMSO
55%


296
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


297
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP1R3
1.0
3.0
22
66
DMSO
55%


298
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP1R5
1.0
5.4
22
119
DMSO
55%


299
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP2R1
2.0
1.3
45
58
DMSO
55%


300
4.0
8%
P6R2
6.0
1.6
136
218
32%
dP2R5
2.0
5.3
45
237
DMSO
55%


301
0.0
40% 
P2R3
2.0
3.5
45
157
 0%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


302
0.05
38% 
P2R3
2.0
3.5
45
157
 2%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


303
0.11
36% 
P2R3
2.0
3.5
45
157
 4%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


304
0.25
32% 
P2R3
2.0
3.5
45
157
 8%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


305
1.00
20% 
P2R3
2.0
3.5
45
157
20%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


306
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


307
9.0
4%
P2R3
2.0
3.5
45
157
36%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


308
19.0
2%
P2R3
2.0
3.5
45
157
38%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


309

0%
P2R3
2.0
3.5
45
157
40%
dP0.4R6
0.4
5.8
7
42
DMSO
55%


310
0.0
40% 
P2R3
2.0
3.5
45
157
 0%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


311
0.05
38% 
P2R3
2.0
3.5
45
157
 2%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


312
0.11
36% 
P2R3
2.0
3.5
45
157
 4%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


313
0.25
32% 
P2R3
2.0
3.5
45
157
 8%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


314
1.00
20% 
P2R3
2.0
3.5
45
157
20%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


315
4.0
8%
P2R3
2.0
3.5
45
157
32%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


316
9.0
4%
P2R3
2.0
3.5
45
157
36%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


317
19.0
2%
P2R3
2.0
3.5
45
157
38%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


318

0%
P2R3
2.0
3.5
45
157
40%
dP0.6R5
0.6
4.6
12
54
DMSO
55%


319
0.0
40% 
P0.4R8
0.4
7.7
9
67
 0%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


320
0.05
38% 
P0.4R8
0.4
7.7
9
67
 2%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


321
0.11
36% 
P0.4R8
0.4
7.7
9
67
 4%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


322
0.25
32% 
P0.4R8
0.4
7.7
9
67
 8%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


323
1.00
20% 
P0.4R8
0.4
7.7
9
67
20%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


324
4.0
8%
P0.4R8
0.4
7.7
9
67
32%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


325
9.0
4%
P0.4R8
0.4
7.7
9
67
36%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


326
19.0
2%
P0.4R8
0.4
7.7
9
67
38%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


327

0%
P0.4R8
0.4
7.7
9
67
40%
dP0.4R8
0.4
8.4
7
61
DMSO
55%


328
0.0
40% 
P1R2
1.0
2.1
22
47
 0%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


329
0.05
38% 
P1R2
1.0
2.1
22
47
 2%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


330
0.11
36% 
P1R2
1.0
2.1
22
47
 4%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


331
0.25
32% 
P1R2
1.0
2.1
22
47
 8%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


332
1.00
20% 
P1R2
1.0
2.1
22
47
20%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


333
4.0
8%
P1R2
1.0
2.1
22
47
32%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


334
9.0
4%
P1R2
1.0
2.1
22
47
36%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


335
19.0
2%
P1R2
1.0
2.1
22
47
38%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


336

0%
P1R2
1.0
2.1
22
47
40%
dP0.6R5
0.6
5.1
12
60
DMSO
55%


337
0.0
40% 
P2R5
2.0
4.8
45
216
 0%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


338
0.05
38% 
P2R5
2.0
4.8
45
216
 2%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


339
0.11
36% 
P2R5
2.0
4.8
45
216
 4%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


340
0.25
32% 
P2R5
2.0
4.8
45
216
 8%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


341
1.00
20% 
P2R5
2.0
4.8
45
216
20%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


342
4.0
8%
P2R5
2.0
4.8
45
216
32%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


343
9.0
4%
P2R5
2.0
4.8
45
216
36%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


344
19.0
2%
P2R5
2.0
4.8
45
216
38%
dP0.2R13
0.2
13.0
3
39
DMSO
55%


345

0%
P2R5
2.0
4.8
45
216
40%
dP0.2R13
0.2
13.0
3
39
DMSO
55%









Example 5—Buprenorphine's Formulations Preparation

The formulations described herein were based on organic solution of polymers prepared as in Example 1, containing as the drug, buprenorphine. Typically, 0.4 grams of polymers, corresponding to a mix of a diblock copolymer and a triblock copolymer in defined mass ratio, were dissolved in 0.5 grams of dimethyl sulfoxide at room temperature overnight under constant magnetic stirring. The next day, 100 mg of buprenorphine was added to the polymer solution and stirred until complete dissolution. The formulations were loaded in a syringe before use.


Three different formulations were selected for in vivo experiments. The composition of these formulations is shown in Table 3 below. The formulations were injected subcutaneously in the interscapular space of male rats (200-250 gr) at a final dose of 100 mg/kg of buprenorphine. Blood samples were withdraw periodically and analyzed for buprenorphine concentrations by LC/MS/MS.


The formulations are shown in Table 3 below.













TABLE 3









Triblock copolymer (TB)
Diblock copolymer (DB)
Solvent






















Exp
Ratio
%

PEG
Ratio
DP-
DP-
%

PEG
Ratio
DP-
DP-

%


no
DB/TB
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
Name
(w/w)

























1
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP0.4R10
0.35
9.8
8
78
DMSO
40.0%


2
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP0.4R10
0.35
9.8
8
78
DMSO
40.0%


3
4.0
10.0%
P2R3
2
3.3
45
150
40.0%
dP0.4R10
0.35
9.8
8
78
DMSO
40.0%


4
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP0.4R10
0.35
9.8
8
78
DMSO
40.0%


5
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP1R4
1
4.2
23
95
DMSO
40.0%


6
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP1R4
1
4.2
23
95
DMSO
40.0%


7
4.0
10.0%
P2R3
2
3.3
45
150
40.0%
dP1R4
1
4.2
23
95
DMSO
40.0%


8
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP1R4
1
4.2
23
95
DMSO
40.0%


9
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP1R5
1
5.4
23
123
DMSO
40.0%


10
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP1R5
1
5.4
23
123
DMSO
40.0%


11
4.0
10.0%
P2R3
2
3.3
45
150
40.0%
dP1R5
1
5.4
23
123
DMSO
40.0%


12
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP1R5
1
5.4
23
123
DMSO
40.0%


13
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP2R3
2
2.7
45
120
DMSO
40.0%


14
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP2R3
2
2.7
45
120
DMSO
40.0%


15
4.0
10.0%
P2R3
2
3.3
45
150
40.0%
dP2R3
2
2.7
45
120
DMSO
40.0%


16
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R3
2
2.7
45
120
DMSO
40.0%


17
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP2R4
2
4.1
45
186
DMSO
40.0%


18
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP2R4
2
4.1
45
186
DMSO
40.0%


19
4.0
10.0%
P2R3
2
3.3
45
150
40.0%
dP2R4
2
4.1
45
186
DMSO
40.0%


20
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R4
2
4.1
45
186
DMSO
40.0%


21
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP2R5
2
5.3
45
241
DMSO
40.0%


22
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP2R5
2
5.3
45
241
DMSO
40.0%


23
4.0
10.0%
P2R3
2
3.3
45
150
40.0%
dP2R5
2
5.3
45
241
DMSO
40.0%


24
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R5
2
5.3
45
241
DMSO
40.0%


26
4.0
9.0%
P0.4R8
0.4
7.7
9
70
36.0%
dP0.4R10
0.35
9.8
8
78
DMSO
45.0%


27
4.0
9.0%
P2R2
2
2.2
45
101
36.0%
dP0.4R10
0.35
9.8
8
78
DMSO
45.0%


28
4.0
9.0%
P2R3
2
3.3
45
150
36.0%
dP0.4R10
0.35
9.8
8
78
DMSO
45.0%


29
4.0
9.0%
P0.4R8
0.4
7.7
9
70
36.0%
dP1R4
1
4.2
23
95
DMSO
45.0%


30
4.0
9.0%
P2R2
2
2.2
45
101
36.0%
dP1R4
1
4.2
23
95
DMSO
45.0%


31
4.0
9.0%
P2R2
2
2.2
45
101
36.0%
dP2R3
2
2.7
45
120
DMSO
45.0%


32
4.0
8.0%
P0.4R8
0.4
7.7
9
70
32.0%
dP0.4R10
0.35
9.8
8
78
DMSO
50.0%


33
4.0
8.0%
P2R2
2
2.2
45
101
32.0%
dP0.4R10
0.35
9.8
8
78
DMSO
50.0%


34
4.0
8.0%
P2R3
2
3.3
45
150
32.0%
dP0.4R10
0.35
9.8
8
78
DMSO
50.0%


35
4.0
8.0%
P0.4R8
0.4
7.7
9
70
32.0%
dP1R4
1
4.2
23
95
DMSO
50.0%


36
4.0
8.0%
P2R2
2
2.2
45
101
32.0%
dP1R4
1
4.2
23
95
DMSO
50.0%


37
4.0
8.0%
P2R2
2
2.2
45
101
32.0%
dP2R3
2
2.7
45
120
DMSO
50.0%


38
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP1R3
1
2.7
23
61
DMSO
40.0%


39
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP1R3
1
2.7
23
61
DMSO
40.0%


40
4.0
10.0%
P2R3
2
3.3
45
150
40.0%
dP1R3
1
2.7
23
61
DMSO
40.0%


41
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP1R3
1
2.7
23
61
DMSO
40.0%


42
4.0
9.0%
P0.4R8
0.4
7.7
9
70
36.0%
dP1R3
1
2.7
23
61
DMSO
45.0%


43
4.0
9.0%
P2R2
2
2.2
45
101
36.0%
dP1R3
1
2.7
23
61
DMSO
45.0%


44
4.0
9.0%
P2R3
2
3.3
45
150
36.0%
dP1R3
1
2.7
23
61
DMSO
45.0%


45
4.0
9.0%
P2R4
2
4.3
45
195
36.0%
dP1R3
1
2.7
23
61
DMSO
45.0%


46
4.0
8.0%
P0.4R8
0.4
7.7
9
70
32.0%
dP1R3
1
2.7
23
61
DMSO
50.0%


47
4.0
8.0%
P2R2
2
2.2
45
101
32.0%
dP1R3
1
2.7
23
61
DMSO
50.0%


48
4.0
8.0%
P2R3
2
3.3
45
150
32.0%
dP1R3
1
2.7
23
61
DMSO
50.0%


49
4.0
8.0%
P2R4
2
4.3
45
195
32.0%
dP1R3
1
2.7
23
61
DMSO
50.0%


51
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP0.4R8
0.35
7.9
8
63
DMSO
40.0%


52
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP0.4R5
0.35
4.9
8
39
DMSO
40.0%


53
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP1R2
1
2.1
23
48
DMSO
40.0%


54
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP2R0.8
2
0.8
45
34
DMSO
40.0%


55
4.0
10.0%
P2R2
2
2.2
45
101
40.0%
dP2R2
2
1.5
45
68
DMSO
40.0%


56
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP0.4R8
0.35
7.9
8
63
DMSO
40.0%


57
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP0.4R5
0.35
4.9
8
39
DMSO
40.0%


58
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP1R2
1
2.1
23
48
DMSO
40.0%


59
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP2R0.8
2
0.8
45
34
DMSO
40.0%


60
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP2R2
2
1.5
45
68
DMSO
40.0%


61
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP0.4R10
0.35
9.8
8
78
DEGMEE
40.0%


62
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP0.4R10
0.35
9.8
8
78
DEGMEE
40.0%


63
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP1R3
1
2.7
23
61
DEGMEE
40.0%


64
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP1R3
1
2.7
23
61
DEGMEE
40.0%


65
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP2R4
2
4.1
45
186
DEGMEE
40.0%


66
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R4
2
4.1
45
186
DEGMEE
40.0%


67
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP0.4R10
0.35
9.8
8
78
Diglyme
40.0%


68
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP0.4R10
0.35
9.8
8
78
Diglyme
40.0%


69
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP1R3
1
2.7
23
61
Diglyme
40.0%


70
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP1R3
1
2.7
23
61
Diglyme
40.0%


71
4.0
10.0%
P0.4R8
0.4
7.7
9
70
40.0%
dP2R4
2
4.1
45
186
Diglyme
40.0%


72
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R4
2
4.1
45
186
Diglyme
40.0%


73
4.0
9.0%
P0.4R8
0.4
7.7
9
70
36.0%
dP1R2
1
2.1
23
48
DMSO
45.0%


74
4.0
8.0%
P0.4R8
0.4
7.7
9
70
32.0%
dP1R2
1
2.1
23
48
DMSO
50.0%


75
3.0
10.0%
P0.4R8
0.4
7.7
9
70
30.0%
dP1R2
1
2.1
23
48
DMSO
50.0%


76
6.0
5.7%
P0.4R8
0.4
7.7
9
70
34.3%
dP1R2
1
2.1
23
48
DMSO
50.0%


77
4.0
8.0%
P0.4R5
0.4
4.7
9
43
32.0%
dP1R2
1
2.1
23
48
DMSO
50.0%


78
4.0
8.0%
P1R2
1
2.1
23
48
32.0%
dP1R2
1
2.1
23
48
DMSO
50.0%


79
4.0
8.0%
P1R3
1
2.8
23
64
32.0%
dP1R2
1
2.1
23
48
DMSO
50.0%


80
4.0
8.0%
P0.4R5
0.4
4.7
9
43
32.0%
dP1R3
1
2.7
23
61
DMSO
50.0%


81
4.0
8.0%
P1R2
1
2.1
23
48
32.0%
dP1R3
1
2.7
23
61
DMSO
50.0%


82
4.0
8.0%
P1R3
1
2.8
23
64
32.0%
dP1R3
1
2.7
23
61
DMSO
50.0%


83
4.0
8.0%
P0.4R5
0.4
4.7
9
43
32.0%
dP0.4R5
0.35
4.9
8
39
DMSO
50.0%


84
4.0
8.0%
P1R2
1
2.1
23
48
32.0%
dP0.4R5
0.35
4.9
8
39
DMSO
50.0%


85
4.0
8.0%
P1R3
1
2.8
23
64
32.0%
dP0.4R5
0.35
4.9
8
39
DMSO
50.0%


86
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R4
2
4.1
45
186
DEGMEE
40.0%


87
4.0
8.0%
P0.4R5
0.4
4.7
9
43
32.0%
dP1R2
1
2.1
23
48
DEGMEE
50.0%


88
4.0
8.0%
P1R2
1
2.1
23
48
32.0%
dP1R2
1
2.1
23
48
DEGMEE
50.0%


89
4.0
8.0%
P1R3
1
2.8
23
64
32.0%
dP1R2
1
2.1
23
48
DEGMEE
50.0%


90
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R4
2
4.1
45
186
Diglyme
40.0%


91
4.0
8.0%
P0.4R5
0.4
4.7
9
43
32.0%
dP1R2
1
2.1
23
48
Diglyme
50.0%


92
4.0
8.0%
P1R2
1
2.1
23
48
32.0%
dP1R2
1
2.1
23
48
Diglyme
50.0%


93
4.0
8.0%
P1R3
1
2.8
23
64
32.0%
dP1R2
1
2.1
23
48
Diglyme
50.0%


95
4.0
10.0%
P2R4
2
4.3
45
195
40.0%
dP2R4
2
4.1
45
186
DMSO
40.0%


96
4.0
8.0%
P0.4R5
0.4
4.7
9
43
32.0%
dP1R2
1
2.1
23
48
DMSO
50.0%


97
4.0
8.0%
P1R2
1
2.1
23
48
32.0%
dP1R2
1
2.1
23
48
DMSO
50.0%


98
4.0
8.0%
P1R3
1
2.8
23
64
32.0%
dP1R2
1
2.1
23
48
DMSO
50.0%









The results of these formulations are illustrated in FIGS. 30 and 31.


Example 6—Risperidone's Formulations Preparation

The formulations described herein were based on organic solution of polymers prepared as in Example 1, containing as the drug, risperidone. Typically, 0.4 grams of polymers, corresponding to a mix of a diblock copolymer and a triblock copolymer in defined mass ratio, were dissolved in 0.5 grams of dimethyl sulfoxide at room temperature overnight under constant magnetic stirring. The next day, 100 mg of risperidone was added to the polymer solution and stirred. The formulations were loaded in a syringe before use.


Three different formulations were selected for in vivo experiments. The composition of these formulations is shown in Table 4 below. The formulations were injected subcutaneously in the interscapular space of male rats (300 gr) at a final dose of 21 mg/kg of risperidone. Blood samples were withdraw periodically and analyzed for risperidone and 9-OH risperidone concentrations by LC/MS/MS.


The formulations are shown in Table 4 below.














TABLE 4









Risp
Triblock copolymer (TB)
Diblock copolymer (DB)
Solvent























Exp
Ratio
%
%

PEG
Ratio
DP-
DP-
%

PEG
Ratio
DP-
DP-

%


no
DB/TB
(w/w)
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
Name
(w/w)


























5
1.5
2.5%
16.0%
P2R3
2
3.5
45
158.6
24.0%
dP2R3
2
2.7
45
122.7
DMSO
57.5%


6
1.5
2.5%
16.0%
P2R2
2
2.3
45
104.5
24.0%
dP1R3
1
2.7
23
61.4
DMSO
57.5%


10
1.5
5.0%
16.0%
P2R2
2
2.3
45
104.5
24.0%
dP2R3
2
2.7
45
122.7
DMSO
55.0%


11
1.5
5.0%
16.0%
P2R3
2
3.5
45
158.6
24.0%
dP2R3
2
2.7
45
122.7
DMSO
55.0%


12
1.5
5.0%
16.0%
P2R2
2
2.3
45
104.5
24.0%
dP1R3
1
2.7
23
61.4
DMSO
55.0%


16
0.7
5.0%
24.0%
P2R3
2
3.5
45
158.6
16.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
55.0%


17
1.5
5.0%
16.0%
P3R2
3
2.3
68
156.8
24.0%
dP2R3
2
2.9
45
131.8
DMSO
55.0%


19
1.5
5.0%
16.0%
P3R3
3
3.2
68
218.2
24.0%
dP2R3
2
2.7
45
122.7
DMSO
55.0%


20
1.5
5.0%
16.0%
P1R4
1
3.8
23
86.4
24.0%
dP2R3
2
2.9
45
131.8
DMSO
55.0%


21
0.7
5.0%
24.0%
P1R4
1
3.8
23
86.4
16.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
55.0%


22
1.5
10.0%
16.0%
P2R2
2
2.3
45
104.5
24.0%
dP2R3
2
2.7
45
122.7
DMSO
50.0%


23
1.5
10.0%
16.0%
P2R3
2
3.5
45
158.6
24.0%
dP2R3
2
2.7
45
122.7
DMSO
50.0%


25
0.7
10.0%
24.0%
P2R3
2
3.5
45
158.6
16.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
50.0%


26
1.5
10.0%
16.0%
P3R3
3
3.2
68
218.2
24.0%
dP2R3
2
2.7
45
122.7
DMSO
50.0%


27
1.5
10.0%
16.0%
P1R4
1
3.8
23
86.4
24.0%
dP2R3
2
2.9
45
131.8
DMSO
50.0%


28
0.7
5.0%
18.0%
P1R4
1
3.8
23
86.4
12.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
65.0%


29
0.7
10.0%
24.0%
P1R4
1
3.8
23
86.4
16.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
60.0%


30
0.7
10.0%
18.0%
P1R4
1
3.8
23
86.4
12.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
60.0%


31
0.7
10.0%
18.0%
P2R3
2
3.5
45
158.6
12.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
60.0%


32
1.5
10.0%
12.0%
P1R4
1
3.8
23
86.4
18.0%
dP2R3
2
2.9
45
131.8
DMSO
60.0%


33
1.5
10.0%
12.0%
P3R3
3
3.2
68
218.2
18.0%
dP2R3
2
2.7
45
122.7
DMSO
60.0%


34
0.7
15.0%
18.0%
P1R4
1
3.8
23
86.4
12.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
55.0%


35
1.5
15.0%
12.0%
P2R2
2
2.3
45
104.5
18.0%
dP2R3
2
2.7
45
122.7
DMSO
55.0%


36
0.7
15.0%
18.0%
P2R3
2
3.5
45
158.6
12.0%
dP0.4R5
0.35
4.9
8
39.0
DMSO
55.0%


40
0.7
10.0%
24.0%
P1R4
1
3.8
23
86.4
16.0%
dP0.4R5
0.35
5.02
8
39.9
DMSO
60.0%


41
0.7
10.0%
18.0%
P2R3
2
3.5
45
158.6
12.0%
dP0.4R5
0.35
5.02
8
39.9
DMSO
60.0%


42
0.7
10.0%
24.0%
P1R4
1
4.0
23
89.8
16.0%
dP0.4R5
0.35
5.02
8
39.9
DMSO
60.0%


43
0.7
10.0%
24.0%
P1R4
1
3.8
23
86.4
16.0%
dP0.4R5
0.35
5.02
8
39.9
DMSO
60.0%


44
0.7
10.0%
24.0%
P1R4
1
4.0
23
89.8
16.0%
dP0.4R5
0.35
5.02
8
39.9
DMSO
60.0%









The results of these formulations are illustrated in FIGS. 32 and 33.


Example 7—Ivermectin's Formulations Preparation

The formulations described herein were based on organic solution of polymers prepared as in Example 1, containing as the drug, ivermectin. Typically, 0.4 grams of polymers, corresponding to a mix of a diblock copolymer and a triblock copolymer in defined mass ratio, were dissolved in 0.55 grams of dimethyl sulfoxide at room temperature overnight under constant magnetic stirring. The next day, 50 mg of ivermectin was added to the polymer solution and stirred until complete dissolution. Three different formulations were selected for in vivo experiments. The composition of these formulations is shown in Table 5 below. The formulations were injected subcutaneously in the interscapular space of male dogs (10 to 17 kg) at a final dose of 0.6 mg/kg of ivermectin. Blood samples were withdraw periodically and analyzed for ivermectin concentrations by LC/MS/MS.


The formulations are shown in Table 5.














TABLE 5









IVM
Triblock copolymer (TB)
Diblock copolymer (DB)
Solvent























Exp
Ratio
%
%

PEG
Ratio
DP-
DP-
%

PEG
Ratio
DP-
DP-

%


no
DB/TB
(w/w)
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
(w/w)
Code
(kDa)
(LA/EO)
PEG
PLA
Name
(w/w)


























9
1.7
5.0%
15.0%
P3R3
3
3.2
68
218
25.0%
dP0.4R5
0.35
4.9
8
39
DMSO
55.0%


10
1.7
5.0%
15.0%
P2R3
2
3.5
45
159
25.0%
dP2R3
2
2.9
45
132
DMSO
55.0%


11
1.7
5.0%
15.0%
P2R5
2
5.3
45
241
25.0%
dP2R2
2
2.3
45
105
DMSO
55.0%









The results are illustrated in FIG. 34.


Example 8—Methdroxyprogesterone Acetate's Formulations Preparations

The formulations as described herein are based on organic solutions of the polymers as described in Example 1, containing as the drug medroxyprogesterone acetate. Typically 0.4 grams of polymers corresponding to a mix of diblock and triblock copolymer in a defined mass ratio were dissolved in 0.3 grams of DMSO or a combination of DMSO and benzyl alcohol at room temperature overnight with constant magnetic stirring. The next day the polymer solution was filtered through a 0.22 μm filter and 0.3 grams of medroxyprogesterone acetate was added to the filtered polymer solution and stirred until a homogeneous suspension of the drug was obtained. The formulations were loaded into a syringe before use. The compositions are shown in Table 6 below. The formulations were injected subcutaneously in the interscapular space of female dogs (11.4 to 14.1 kg). Blood samples were withdrawn periodically and analyzed for medroxyprogesterone acetate concentrations by LC/MS/MS having a below limit of quantification of 0.25 ng/ml. The results are shown in FIG. 35.


The formulations are shown in Table 6.



















TABLE 6







Exp
Exp.
Experiment
Duration

Drug loading
Polymer
% Polymer 1

Ratio
DP-


no
Code
type
(days)
Drug type
% (w/w)
% (w/w)
TRIBLOCK

(LA/EO)
PEG





1
AR01.01
Dosing curve
9
Medroxyprogesterone


2
AR02.01
Solvent solubility
28
Medroxyprogesterone


3
AR03.01
Buffer solubility
4
Medroxyprogesterone


4
AR04.01
Buffer solubility
15
Medroxyprogesterone


5
AR05.01
In vitro release
195
Medroxyprogesterone
10%
35%
14%
1
3.95
23


6
AR06.01
In vitro release
195
Medroxyprogesterone
20%
35%
14%
1
3.95
23


7
AR07.01
In vitro release
195
Medroxyprogesterone
30%
35%
14%
1
3.95
23


8
AR08.01
In vitro release
195
Medroxyprogesterone
10%
40%
16%
1
3.95
23


9
AR09.01
In vitro release
195
Medroxyprogesterone
20%
40%
16%
1
3.95
23


10
AR10.01
In vitro release
195
Medroxyprogesterone
30%
40%
16%
1
3.95
23


11
BJ01.01
In vitro release
342
Medroxyprogesterone
10%
40%
16%
2
3.49
45


12
BJ02.01
In vitro release
342
Medroxyprogesterone
20%
40%
16%
2
3.49
45


13
BJ03.01
In vitro release
342
Medroxyprogesterone
30%
40%
16%
2
3.49
45


14
AR11.01
In vitro release
146
Depot SubQ Provera


15
AR12.01
In vitro release
189
Medroxyprogesterone
20%
30%
12%
1
3.95
23


16
AR13.01
In vitro release
189
Medroxyprogesterone
20%
30%
18%
1
3.95
23


17
AR14.01
In vitro release
189
Medroxyprogesterone
20%
35%
21%
1
3.95
23


18
AR15.01
In vitro release
189
Medroxyprogesterone
20%
40%
24%
1
3.95
23


19
AR16.01
In vitro release
189
Medroxyprogesterone
20%
30%
18%
2
3.49
45


20
BJ04.01
In vitro release
336
Medroxyprogesterone
20%
40%
24%
2
3.49
45


21
BJ05.01
In vitro release
336
Medroxyprogesterone
20%
30%
12%
2
3.49
45


22
BJ06.01
In vitro release
336
Medroxyprogesterone
20%
35%
14%
2
3.49
45


23
AR17.01
In vitro release
182
Medroxyprogesterone
20%
20%
 8%
1
3.95
23


24
AR18.01
In vitro release
182
Medroxyprogesterone
20%
20%
12%
1
3.95
23


25
AR19.01
In vitro release
182
Medroxyprogesterone
20%
20%
16%
1
3.95
23


26
AR20.01
In vitro release
182
Medroxyprogesterone
20%
20%
12%
2
3.49
45


27
AR21.01
In vitro release
182
Medroxyprogesterone
20%
20%
16%
2
3.49
45


28
AR22.01
In vitro release
182
Medroxyprogesterone
20%
20%
 8%
2
3.49
45


29
BJ07.01
In vitro release
329
Medroxyprogesterone
20%
20%
12%
2
3.49
45


30
BJ08.01
In vitro release
329
Medroxyprogesterone
20%
20%
16%
2
3.49
45


31
BJ09.01
In vitro release
329
Medroxyprogesterone
20%
30%
30%
2
3.49
45


32
BJ10.01
In vitro release
55
Medroxyprogesterone
30%
10%
 6%
2
3.49
45


33
BJ11.01
In vitro release
55
Medroxyprogesterone
40%
 5%
 3%
2
3.49
45


34
BJ12.01
In vitro release
55
Medroxyprogesterone
30%
10%
 6%
2
3.49
45


35
BJ13.01
In vitro release
55
Medroxyprogesterone
30%
10%


36
BJ14.01
In vitro release
309
Medroxyprogesterone
20%
20%
12%
2
3.49
45


37
BJ15.01
In vitro release
309
Medroxyprogesterone
20%
20%
12%
2
3.49
45


38
AR23.01
In vitro release
191
Medroxyprogesterone
20%
20%
12%
2
3.49
45


39
AR24.01
In vitro release
191
Medroxyprogesterone
20%
20%
12%
2
3.49
45


40
AR25.01
In vitro release
191
Medroxyprogesterone
20%
20%
12%
2
3.3
45


41
BJ16.01
In vitro release
49
Medroxyprogesterone
42%


42
BJ17.01
In vitro release
267
Medroxyprogesterone
40%
 5%
 3%
2
3.49
45


43
AR26.01
In Vivo Study
165
Medroxyprogesterone Ir
30%
10%
 6%
2
3.49
45


44
AR27.01
In Vivo Study
165
Medroxyprogesterone Ir
40%
 5%
 3%
2
3.49
45


45
AR28.01
In Vivo Study
165
Medroxyprogesterone Ir
30%
10%
 6%
2
3.49
45


46
AR29.01
In Vivo Study

Medroxyprogesterone Ir
30%
10%
 6%
2
3.49
45


47
AR30.01
In Vivo Study
143
Medroxyprogesterone Ir
20%
20%
12%
2
3.49
45


48
AR31.01
In Vivo Study
190
Medroxyprogesterone Ir
20%
40%
16%
2
3.74
45


49
AR32.01
In Vivo Study
115
Medroxyprogesterone Ir
20%
10%
 6%
2
3.74
45


50
AR33.01
Solvent Solubility
2
Medroxyprogesterone


51
AR34.01
Dosing curve
2
Medroxyprogesterone


52
AR35.01
In vitro release
111
Medroxyprogesterone Ir
40%
 5%
 3%
2
3.6
45


53
AR36.01
In vitro release
111
Medroxyprogesterone Ir
30%
10%
 6%
2
3.6
45


54
AR37.01
In vitro release
111
Medroxyprogesterone Ir
20%
10%
 6%
2
3.6
45


55
AR38.01
In vitro release
111
Depot SubQ Provera


56
AR39.01
In vitro release
64
Medroxyprogesterone Ir
30%
10%
 6%
2
3.6
45


57
AR40.01
In vitro release
64
Medroxyprogesterone Ir
20%
10%
 6%
2
3.6
45


58
AR41.01
In vitro release
96
Medroxyprogesterone
40%
 5%
 3%
2
3.6
45


59
AR42.01
In vitro release
96
Medroxyprogesterone
40%
 5%
 3%
2
3.6
45


60
AR43.01
In vitro release
96
Medroxyprogesterone
20%
10%
 6%
2
3.6
45


61
AR44.01
In vitro release
96
Medroxyprogesterone
20%
10%
 6%
2
3.6
45


62
AR45.01
Solvent Solubility
1
Medroxyprogesterone


63
AR46.01
In vitro release
50
Medroxyprogesterone Ir
30%
10%
 6%
2
3.6
45


64
AR47.01
In vitro release
50
Medroxyprogesterone Ir
20%
10%
 6%
2
3.6
45
































Solubilisation


Exp
DP-
% Polymer 2
PEG
Ratio
DP-
DP-

% Solvent 1

% Solvent 2
Time Org


no
PLA
DIBLOCK
(kDa)
(LA/EO)
PEG
PLA
Solvent 1
(w/w)
Solvent 2
(w/w°
phase





1


2


3


4


5
89.8
21% 
0.35
5.02
8
39.9
DMSO
55%


Stir Overnight













@Room Temp


6
89.8
21% 
0.35
5.02
8
39.9
DMSO
45%


Stir Overnight













@Room Temp


7
89.8
21% 
0.35
5.02
8
39.9
DMSO
35%


Stir Overnight













@Room Temp


8
89.8
24% 
0.35
5.02
8
39.9
DMSO
50%


Stir Overnight













@Room Temp


9
89.8
24% 
0.35
5.02
8
39.9
DMSO
40%


Stir Overnight













@Room Temp


10
89.8
24% 
0.35
5.02
8
39.9
DMSO
30%


Stir Overnight













@Room Temp


11
158.6
24% 
2
2.7
45
122.7
DMSO
50%


Stir Overnight













@Room Temp


12
158.6
24% 
2
2.7
45
122.7
DMSO
40%


Stir Overnight













@Room Temp


13
158.6
24% 
2
2.7
45
122.7
DMSO
30%


Stir Overnight













@Room Temp


14


15
89.8
18% 
0.35
5.02
8
39.9
DMSO
50%


Stir Overnight













@Room Temp


16
89.8
12% 
0.35
5.02
8
39.9
DMSO
50%


Stir Overnight













@Room Temp


17
89.8
14% 
0.35
5.02
8
39.9
DMSO
45%


Stir Overnight













@Room Temp


18
89.8
16% 
0.35
5.02
8
39.9
DMSO
40%


Stir Overnight













@Room Temp


19
158.6
12% 
0.35
5.02
8
39.9
DMSO
50%


Stir Overnight













@Room Temp


20
158.6
16% 
0.35
5.02
8
39.9
DMSO
40%


Stir Overnight













@Room Temp


21
158.6
18% 
2
2.7
45
122.7
DMSO
50%


Stir Overnight













@Room Temp


22
158.6
21% 
2
2.7
45
122.7
DMSO
45%


Stir Overnight













@Room Temp


23
89.8
12% 
0.35
5.02
8
39.9
DMSO
60%


Stir Overnight













@Room Temp


24
89.8
8%
0.35
5.02
8
39.9
DMSO
60%


Stir Overnight













@Room Temp


25
89.8
4%
0.35
5.02
8
39.9
DMSO
60%


Stir Overnight













@Room Temp


26
158.6
8%
0.35
5.02
8
39.9
DMSO
60%


Stir Overnight













@Room Temp


27
158.6
4%
0.35
5.02
8
39.9
DMSO
60%


Stir Overnight













@Room Temp


28
158.6
12% 
2
2.7
45
122.7
DMSO
60%


Stir Overnight













@Room Temp


29
158.6
8%
2
2.7
45
122.7
DMSO
60%


Stir Overnight













@Room Temp


30
158.6
4%
2
2.7
45
122.7
DMSO
60%


Stir Overnight













@Room Temp


31
158.6





DMSO
60%


Stir Overnight













@Room Temp


32
158.6
4%
2
2.7
45
122.7
DMSO
60%


Stir Overnight













@Room Temp


33
158.6
2%
2
2.7
45
122.7
DMSO
55%


Stir Overnight













@Room Temp


34
158.6
4%
2
2.7
45
122.7
DMSO
30%
Benzyl Alcohol
30%
Stir Overnight













@Room Temp


35

10% 
2
2.7
45
122.7
DMSO
60%


Stir Overnight













@Room Temp


36
158.6
8%
0.35
5.02
8
39.9
DMSO
30%
Benzyl Alcohol
30%
Stir Overnight













@Room Temp


37
158.6
8%
0.35
5.02
8
39.9
DMSO
45%
Benzyl Alcohol
15%
Stir Overnight













@Room Temp


38
158.6
8%
2
2.7
45
122.7
DMSO
30%
Benzyl Alcohol
30%
Stir Overnight













@Room Temp


39
158.6
8%
2
2.7
45
122.7
DMSO
45%
Benzyl Alcohol
15%
Stir Overnight













@Room Temp


40
150.0
8%
2
2.7
45
122.7
DMSO
30%
Benzyl Alcohol
30%
Stir Overnight













@Room Temp


41






DMSO
58%


42
158.6
2%
2
2.7
45
122.7
DMSO
55%


43
158.6
4%
2
2.7
45
122.7
DMSO
60%


44
158.6
2%
2
2.7
45
122.7
DMSO
55%


45
158.6
4%
2
2.7
45
122.7
DMSO
30%
Benzyl Alcohol
30%


46
158.6
4%
2
2.7
45
122.7
DMSO
60%


47
158.6
8%
0.35
5.02
8
39.9
DMSO
30%
Benzyl Alcohol
30%


48
170.0
24% 
2
2.34
45
106.4
DMSO
40%


49
170.0
4%
2
2.34
45
106.4
DMSO
35%
Benzyl Alcohol
35%


50


51


52
163.6
2%
2
2.48
45
112.7
DMSO
54.5%


53
163.6
4%
2
2.48
45
112.7
DMSO
####
Benzyl Alcohol
####


54
163.6
4%
2
2.48
45
112.7
DMSO
####
Benzyl Alcohol
####


55


56
163.6
4%
2
2.48
45
112.7
DMSO
30.0%
Benzyl Alcohol
30.0%


57
163.6
4%
2
2.48
45
112.7
DMSO
35.0%
Benzyl Alcohol
35.0%


58
163.6
2%
2
2.48
45
112.7
DMSO
54.5%


59
163.6
2%
2
2.48
45
112.7
DMSO
26.0%


60
163.6
4%
2
2.48
45
112.7
DMSO
####
Benzyl Alcohol
####


61
163.6
4%
2
2.48
45
112.7
DMSO
20.5%
Benzyl Alcohol
20.5%


62






DMSO


63
163.6
4%
2
2.48
45
112.7
DMSO
30.0%
Benzyl Alcohol
30.0%


64
163.6
4%
2
2.48
45
112.7
DMSO
35.0%
Benzyl Alcohol
35.0%










DRUG: MEDROXYPROGESTERONE (MPA)


















Exp
Drug loading
Polymer
Ratio

Polymer 1
Batch
PEG
Ratio
DP-
DP-



no
% (w/w)
% (w/w)
Pol1/Pol2
% Polymer 1
code
number
(kDa)
(LA/EO)
PEG
PLA
% Polymer 2





5
10%
35%
0.7
14%
P1R4
MIC180-C
1
4.0
23
90
21%


6
20%
35%
0.7
14%
P1R4
MIC180-C
1
4.0
23
90
21%


7
30%
35%
0.7
14%
P1R4
MIC180-C
1
4.0
23
90
21%


8
10%
40%
0.7
16%
P1R4
MIC180-C
1
4.0
23
90
24%


9
20%
40%
0.7
16%
P1R4
MIC180-C
1
4.0
23
90
24%


10
30%
40%
0.7
16%
P1R4
MIC180-C
1
4.0
23
90
24%


11
10%
40%
0.7
16%
P2R3
MIC166-C
2
3.5
45
159
24%


12
20%
40%
0.7
16%
P2R3
MIC166-C
2
3.5
45
159
24%


13
30%
40%
0.7
16%
P2R3
MIC166-C
2
3.5
45
159
24%


15
20%
30%
0.7
12%
P1R4
MIC180-C
1
4.0
23
90
18%


16
20%
30%
1.5
18%
P1R4
MIC180-C
1
4.0
23
90
12%


17
20%
35%
1.5
21%
P1R4
MIC180-C
1
4.0
23
90
14%


18
20%
40%
1.5
24%
P1R4
MIC180-C
1
4.0
23
90
16%


19
20%
30%
1.5
18%
P2R3
MIC166-C
2
3.5
45
159
12%


20
20%
40%
1.5
24%
P2R3
MIC166-C
2
3.5
45
159
16%


21
20%
30%
0.7
12%
P2R3
MIC166-C
2
3.5
45
159
18%


22
20%
35%
0.7
14%
P2R3
MIC166-C
2
3.5
45
159
21%


23
20%
20%
0.7
 8%
P1R4
MIC180-C
1
4.0
23
90
12%


24
20%
20%
1.5
12%
P1R4
MIC180-C
1
4.0
23
90
 8%


25
20%
20%
4.0
16%
P1R4
MIC180-C
1
4.0
23
90
 4%


26
20%
20%
1.5
12%
P2R3
MIC166-C
2
3.5
45
159
 8%


27
20%
20%
4.0
16%
P2R3
MIC166-C
2
3.5
45
159
 4%


28
20%
20%
0.7
 8%
P2R3
MIC166-C
2
3.5
45
159
12%


29
20%
20%
1.5
12%
P2R3
MIC166-C
2
3.5
45
159
 8%


30
20%
20%
4.0
16%
P2R3
MIC166-C
2
3.5
45
159
 4%


32
30%
10%
1.5
 6%
P2R3
MIC166-C
2
3.5
45
159
 4%


33
40%
 5%
1.5
 3%
P2R3
MIC166-C
2
3.5
45
159
 2%


34
30%
10%
1.5
 6%
P2R3
MIC166-C
2
3.5
45
159
 4%


36
20%
20%
1.5
12%
P2R3
MIC166-C
2
3.5
45
159
 8%


37
20%
20%
1.5
12%
P2R3
MIC166-C
2
3.5
45
159
 8%


38
20%
20%
1.5
12%
P2R3
MIC166-C
2
3.5
45
159
 8%


39
20%
20%
1.5
12%
P2R3
MIC166-C
2
3.5
45
159
 8%


40
20%
20%
1.5
12%
P2R3
MIC205
2
3.3
45
150
 8%


41
42%


42
40%
 5%
1.5
 3%
P2R3
MIC166-C
2
3.5
45
159
 2%


58
40%
 5%
1.5
 3%
P2R4
MIC227
2
3.6
45
164
 2%


59
40%
 5%
1.5
 3%
P2R4
MIC227
2
3.6
45
164
 2%


60
20%
10%
1.5
 6%
P2R4
MIC227
2
3.6
45
164
 4%


61
20%
10%
1.5
 6%
P2R4
MIC227
2
3.6
45
164
 4%






















Exp
Polymer 2
Batch
PEG
Ratio
DP-
DP-

% Solvent 1

% Solvent 2



no
code
number
(kDa)
(LA/EO)
PEG
PLA
Solvent 1
(w/w)
Solvent 2
(w/w)







5
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
55.0%



6
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
45.0%



7
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
35.0%



8
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
50.0%



9
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
40.0%



10
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
30.0%



11
dP2R3
MIC138-A
2
2.7
45
123
DMSO
50.0%



12
dP2R3
MIC138-A
2
2.7
45
123
DMSO
40.0%



13
dP2R3
MIC138-A
2
2.7
45
123
DMSO
30.0%



15
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
50.0%



16
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
50.0%



17
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
45.0%



18
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
40.0%



19
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
50.0%



20
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
40.0%



21
dP2R3
MIC138-A
2
2.7
45
123
DMSO
50.0%



22
dP2R3
MIC138-A
2
2.7
45
123
DMSO
45.0%



23
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
60.0%



24
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
60.0%



25
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
60.0%



26
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
60.0%



27
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
60.0%



28
dP2R3
MIC138-A
2
2.7
45
123
DMSO
60.0%



29
dP2R3
MIC138-A
2
2.7
45
123
DMSO
60.0%



30
dP2R3
MIC138-A
2
2.7
45
123
DMSO
60.0%



32
dP2R3
MIC138-A
2
2.7
45
123
DMSO
60.0%



33
dP2R3
MIC138-A
2
2.7
45
123
DMSO
55.0%



34
dP2R3
MIC138-A
2
2.7
45
123
DMSO
30.0%
Benzyl
30.0%












Alcohol



36
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
30.0%
Benzyl
30.0%












Alcohol



37
dP0.35R5
MIC173-C1
0.35
5.0
8
40
DMSO
45.0%
Benzyl
15.0%












Alcohol



38
dP2R3
MIC138-A
2
2.7
45
123
DMSO
30.0%
Benzyl
30.0%












Alcohol



39
dP2R3
MIC138-A
2
2.7
45
123
DMSO
45.0%
Benzyl
15.0%












Alcohol



40
dP2R3
MIC138-A
2
2.7
45
123
DMSO
30.0%
Benzyl
30.0%












Alcohol



41






DMSO
58.0%



42
dP2R3
MIC138-A
2
2.7
45
123
DMSO
55.0%



58
dP2R2
MIC226
2
2.5
45
113
DMSO
54.5%



59
dP2R2
MIC226
2
2.5
45
113
DMSO
26.0%



60
dP2R2
MIC226
2
2.5
45
113
DMSO
34.8%
Benzyl
34.8%












Alcohol



61
dP2R2
MIC226
2
2.5
45
113
DMSO
20.5%
Benzyl
20.5%












Alcohol










Example 9—Progesterone Formulations Preparations

The formulations as described herein are based on organic solutions of the polymers as described in Example 1, containing as the drug progesterone. Typically 0.1 grams of polymers corresponding to a mix of diblock and triblock copolymer in a defined mass ratio were dissolved in 0.6 grams of DMSO at room temperature overnight with constant magnetic stirring. The next day the polymer solution was filtered through a 0.22 μm filter and 0.3 grams of progesterone was added to the filtered polymer solution and stirred until a homogeneous suspension of the drug was obtained. The formulations were loaded into a syringe before use. The compositions are shown in Table 7 below.









TABLE 7





DRUG: PROGESTERONE
























Exp
Drug loading
Polymer
Ratio
% Polymer 1 -
Polymer 1
Batch
PEG
Ratio
DP-


no
% (w/w)
% (w/w)
Pol1/Pol2
Triblock
code
number
(kDa)
(LA/EO)
PEG





2
20%
40%
0.7
 16%
P1R3
MIC239-C
2
3.5
45


3
30%
10%
1.5

6%

P1R3
MIC239-C
2
3.5
45


4
20%
20%
1.5
 12%
P1R3
MIC239-C
2
3.5
45


5
40%
 5%
1.5
3.0%
P1R3
MIC239-C
2
3.5
45


6
30%
10%
1.5

6%

P1R3
MIC239-C
2
3.5
45


7
20%
10%
1.5
6.0%
P1R3
MIC239-C
2
3.5
45


10
40%
 0%


11
20%
 0%


12
40%
2.5% 
1.5
1.5%
P1R3
MIC239-C
2
3.5
45


13
20%
 5%
1.5
3.0%
P1R3
MIC239-C
2
3.5
45






























%


Exp
DP-
% Polymer 2 -
Polymer 2
Batch
PEG
Ratio
DP-
DP-

Solvent 1


no
PLA
Diblock
code
number
(kDa)
(LA/EO)
PEG
PLA
Solvent 1
(w/w)





2
159
 24%
dP2R2
MIC238
2
2.3
45
106
DMSO
40.0%


3
159

4%

dP2R2
MIC238
2
2.3
45
106
DMSO
60.0%


4
158

8%

dP0.35R5
MIC251-C
0.35
5.4
8
43
DMSO
60.0%


5
159
2.0%
dP2R2
MIC238
2
2.3
45
106
DMSO
55.0%


6
159

4%

dP2R2
MIC238
2
2.3
45
106
DMSO
60.0%


7
158
4.0%
dP2R2
MIC238
2
2.3
45
106
DMSO
70.0%


10








DMSO
60.0%


11








DMSO
80.0%


12
159
1.0%
dP2R2
MIC238
2
2.3
45
106
DMSO
57.5%


13
158
2.0%
dP2R2
MIC238
2
2.3
45
106
DMSO
75.0%









Example 10—Levonorgestrel Formulations Preparations

The formulations as described herein are based on organic solutions of the polymers as described in Example 1, containing as the drug Levonorgestrel. Typically 0.1 grams of polymers corresponding to a mix of diblock and triblock copolymer in a defined mass ratio were dissolved in 0.7 grams of DMSO at room temperature overnight with constant magnetic stirring. The next day the polymer solution was filtered through a 0.22 μm filter and 0.2 grams [of Levonorgestrel was added to the filtered polymer solution and stirred until a homogeneous suspension of the drug was obtained. The formulations were loaded into a syringe before use. The compositions are shown in Table 8 below.









TABLE 8





DRUG: LEVONORGESTREL
























Exp
Drug loading
Polymer
Ratio
% Polymer 1 -
Polymer 1
Batch
PEG
Ratio
DP-


no
% (w/w)
% (w/w)
Pol1/Pol2
Triblock
code
number
(kDa)
(LA/EO)
PEG





4
20%
0%



5
20%
5%
1.5
3%
P2R3
MIC239-C
2
3.5
45


6
20%
10% 
1.5
6%
P2R3
MIC239-C
2
3.5
45


7
10%
0%



8
10%
5%
1.5
3%
P2R3
MIC239-C
2
3.5
45


9
10%
10% 
1.5
6%
P2R3
MIC239-C
2
3.5
45






























%


Exp
DP-
% Polymer 2 -
Polymer 2
Batch
PEG
Ratio
DP-
DP-

Solvent 1


no
PLA
Diblock
code
number
(kDa)
(LA/EO)
PEG
PLA
Solvent 1
(w/w)





4








DMSO
80%


5
158
2%
dP2R2
MIC238
2
2.3
45
106
DMSO
75%


6
158
4%
dP2R2
MIC238
2
2.3
45
106
DMSO
70%


7








DMSO
90%


8
159
2%
dP2R2
MIC238
2
2.3
45
106
DMSO
87.5%


9
159
4%
dP2R2
MIC238
2
2.3
45
106
DMSO
85%









Example 10—Cyclosporine Formulations Preparations

The formulations as described herein are based on organic solutions of the polymers as described in Example 1, containing as the drug cyclosporine. Typically 0.15 grams of polymers corresponding to a mix of diblock and triblock copolymer in a defined mass ratio were dissolved in 0.65 grams of DMSO at room temperature overnight with constant magnetic stirring. The next day the polymer solution was filtered through a 0.22 μm filter and 0.2 grams of cyclosporine was added to the filtered polymer solution and stirred until a homogeneous suspension of the drug was obtained. The formulations were loaded into a syringe before use. The compositions are shown in Table 9 below.









TABLE 9





DRUG: CYCLOSPORINE
























Exp
Drug loading
Polymer
Ratio
% Polymer 1 -
Polymer 1
Batch
PEG
Ratio
DP-


no
% (w/w)
% (w/w)
Pol2/Pol1
Triblock
code
number
(kDa)
(LA/EO)
PEG





12
5.0%
35.0%
4.0
7.0%
P1R4
MIC243-C
1.0
4.0
22


13
5.0%
35.0%
4.0
7.0%
P1R4
MIC243-C
1.0
4.0
22


14
5.0%
35.0%
4.0
7.0%
P1R4
MIC243-C
1.0
4.0
22


16
10.0%
35.0%
4.0
7.0%
P1R4
MIC243-C
1.0
4.0
22


17
12.8%
25.7%
4.0
5.0%
P1R4
MIC243-C
1.0
4.0
22


18
15.9%
20.1%
4.0
4.1%
P1R4
MIC243-C
1.0
4.0
22


19
17.7%
14.2%
4.0
2.9%
P1R4
MIC243-C
1.0
4.0
22


20
18.8%
9.4%
4.0
1.9%
P1R4
MIC243-C
1.0
4.0
22


21
21.1%
6.0%
4.0
1.2%
P1R4
MIC243-C
1.0
4.0
22


22
20.0%
10.0%
4.0
2.0%
P1R4
MIC243-C
1.0
4.0
22


23
20.0%
12.5%
4.0
2.5%
P1R4
MIC243-C
1.0
4.0
22


24
20.0%
15.0%
4.0
3.0%
P1R4
MIC243-C
1.0
4.0
22


25
20.0%
17.5%
4.0
3.5%
P1R4
MIC243-C
1.0
4.0
22






























%


Exp
DP-
% Polymer 2 -
Polymer 2
Batch
PEG
Ratio
DP-
DP-

Solvent 1


no
PLA
Diblock
code
number
(kDa)
(LA/EO)
PEG
PLA
Solvent 1
(w/w)





12
89
28.0%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
60.0%


13
89
28.0%
dP2R2
MIC245-C
2.0
2.5
45
111
DMSO
60.0%


14
89
28.0%
dP0.6R5
MIC187-C
0.55
5.1
12
60
DMSO
60.0%


16
89
28.0%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
55.0%


17
89
20.7%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
61.5%


18
89
16.0%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
64.0%


19
89
11.3%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
68.1%


20
89
7.5%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
71.8%


21
89
4.8%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
72.9%


22
89
8.0%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
70.0%


23
89
10.0%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
67.5%


24
89
12.0%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
65.0%


25
89
14.0%
dP1R4
MIC225-C
1.0
3.9
22
85
DMSO
62.5%









Example 11—Bupivacaine Formulations Preparations

The formulations as described herein are based on organic solutions of the polymers as described in Example 1, containing as the drug Bupivacaine base. Typically 0.1 grams of polymers corresponding to a mix of diblock and triblock copolymer in a defined mass ratio were dissolved in 0.75 grams of DMSO at room temperature overnight with constant magnetic stirring. The next day the polymer solution was filtered through a 0.22 μm filter and 0.15 grams of Bupivacaine base was added to the filtered polymer solution and stirred until a homogeneous suspension of the drug was obtained. The formulations were loaded into a syringe before use. The compositions are shown in Table 10 below.









TABLE 10





DRUG: BUPIVACAINE FORMULATIONS (BUPI)
























Exp
Drug loading
Polymer
Ratio

Polymer 1 -
Batch
PEG
Ratio
DP-


no
% (w/w)
% (w/w)
Pol1/Pol2
% Polymer 1
Triblock code
number
(kDa)
(LA/EO)
PEG





2
  1%
30.0%
2.0
20%
P1R4
MIC243-C
1
4.0
23


3
  1%
30.0%
2.0
20%
P1R4
MIC243-C
1
4.0
23


4
  1%
30.0%
2.0
20%
P2R3
MIC239-C
2
3.5
45


5
  1%
30.0%
2.0
20%
P2R3
MIC239-C
2
3.5
45


6
  1%
30.0%
2.0
20%
P3R2
MIC195-C
3
1.9
68


7
  1%
30.0%
2.0
20%
P3R2
MIC195-C
3
1.9
68


9
 5.0%
30.0%
2.0
20%
P1R4
MIC243-C
1
4.0
23


10
 1.3%
30.0%
1.0
15%
P1R4
MIC243-C
1
4.0
23


11
 1.3%
30.0%
2.0
20%
P1R4
MIC243-C
1
4.0
23


12
 1.3%
30.0%
1.0
15%
P1R4
MIC243-C
1
4.0
23


13
 1.3%
30.0%
2.0
20%
P2R2
MIC230
2
2.4
45


14
 1.3%
30.0%
1.0
15%
P2R2
MIC230
2
2.4
45


15
 1.3%
30.0%
2.0
20%
P2R2
MIC230
2
2.4
45


16
 1.3%
30.0%
1.0
15%
P2R2
MIC230
2
2.4
45


30
 5.0%
30.0%
2.0
20.0%
P1R4
MIC243-C
1
4.0
23


31
 1.0%
30.0%
2.0
20.0%
P1R4
MIC243-C
1
4.0
23


32
 1.0%
30.0%
2.0
20.0%
P2R2
MIC230
2
2.4
45


33
 5.0%
30.0%
1.0
15.0%
P1R4
MIC243-C
1
4.0
23


34
10.0%
30.0%
1.0
15.0%
P1R4
MIC243-C
1
4.0
23


35
10.0%
25.0%
1.0
12.5%
P1R4
MIC243-C
1
4.0
23


36
12.5%
25.0%
1.0
12.5%
P1R4
MIC243-C
1
4.0
23


37
10.0%
20.0%
1.0
10.0%
P1R4
MIC243-C
1
4.0
23


38
12.5%
20.0%
1.0
10.0%
P1R4
MIC243-C
1
4.0
23


39
15.0%
20.0%
1.0
10.0%
P1R4
MIC243-C
1
4.0
23


40
15.0%
20.0%
2.0
13.3%
P1R4
MIC243-C
1
4.0
23


41
12.5%
15.0%
1.0
7.5% 
P1R4
MIC243-C
1
4.0
23


42
10.0%
10.0%
1.0
5.0% 
P1R4
MIC243-C
1
4.0
23


43
12.5%
10.0%
1.0
5.0% 
P1R4
MIC243-C
1
4.0
23


44
15.0%
10.0%
1.0
5.0% 
P1R4
MIC243-C
1
4.0
23


45
12.5%
15.0%
2.0
10.0%
P1R4
MIC243-C
1
4.0
23


46
15.0%
10.0%
2.0
6.7% 
P1R4
MIC243-C
1
4.0
23


47
10.0%
15.0%
1.0
7.5% 
P1R4
MIC243-C
1
4.0
23


48
11.0%
15.0%
1.0
7.5% 
P1R4
MIC243-C
1
4.0
23


49
12.0%
15.0%
1.0
7.5% 
P1R4
MIC243-C
1
4.0
23






























%


Exp
DP-
% Polymer 2 -
Polymer 2
Batch
PEG
Ratio
DP-
DP-

Solvent 1


no
PLA
Diblock
code
number
(kDa)
(LA/EO)
PEG
PLA
Solvent 1
(w/w)





2
91
10%
dP0.35R6
MIC207-C
0.35
5.8
8
46
DMSO
69.0%


3
91
10%
dP2R2
MIC238
2
2.3
45
106
DMSO
69.0%


4
158
10%
dP0.35R6
MIC207-C
0.35
5.8
8
46
DMSO
69.0%


5
158
10%
dP2R2
MIC238
2
2.3
45
106
DMSO
69.0%


6
128
10%
dP0.35R6
MIC207-C
0.35
5.8
8
46
DMSO
69.0%


7
128
10%
dP2R2
MIC238
2
2.3
45
106
DMSO
69.0%


9
91
10%
dP0.35R6
MIC207-C
0.35
5.8
8
46
DMSO
65.0%


10
91
15%
dP0.35R6
MIC207-C
0.35
5.8
8
46
DMSO
68.7%


11
91
10%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
68.7%


12
91
15%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
68.7%


13
110
10%
dP0.35R6
MIC207-C
0.35
5.8
8
46
DMSO
68.7%


14
110
15%
dP0.35R6
MIC207-C
0.35
5.8
8
46
DMSO
68.7%


15
110
10%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
68.7%


16
110
15%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
68.7%


30
91
10.0%
dP0.35R5
MIC251-C
0.35
5.4
8
43
DMSO
65.0%


31
91
10.0%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
69.0%


32
110
10.0%
dP0.35R5
MIC251-C
0.35
5.4
8
43
DMSO
69.0%


33
91
15.0%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
65.0%


34
91
15.0%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
60.0%


35
91
12.5%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
65.0%


36
91
12.5%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
62.5%


37
91
10.0%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
70.0%


38
91
10.0%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
67.5%


39
91
10.0%
dP1R4
MIC225-C
1
3.9
23
88
DMSO
65.0%


40
91
6.7% 
dP2R3
MIC252-C
2
3.0
45
135
DMSO
65.0%


41
91
7.5% 
dP1R4
MIC225-C
1
3.9
23
88
DMSO
72.5%


42
91
5.0% 
dP1R4
MIC225-C
1
3.9
23
88
DMSO
80.0%


43
91
5.0% 
dP1R4
MIC225-C
1
3.9
23
88
DMSO
77.5%


44
91
5.0% 
dP1R4
MIC225-C
1
3.9
23
88
DMSO
75.0%


45
91
5.0% 
dP2R2
MIC238
2
2.3
45
106
DMSO
72.5%


46
91
3.3% 
dP2R2
MIC238
2
2.3
45
106
DMSO
75.0%


47
91
7.5% 
dP1R4
MIC225-C
1
3.9
23
88
DMSO
75.0%


48
91
7.5% 
dP1R4
MIC225-C
1
3.9
23
88
DMSO
74.0%


49
91
7.5% 
dP1R4
MIC225-C
1
3.9
23
88
DMSO
73.0%









Example 12—Injectability of Differing Compositions

Various formulations were tested for injectability using formulations with different ratios of triblock (TB) and diblock (DB). Different solutions in DMSO based on a mixture of the triblock copolymer P6R1(TB) and the diblock copolymer dP2R4(DB) were prepared.


A 50% weight %/weight % polymer/formulation mass was used in these viscosity experiments. The weight %/weight % of triblock to diblock that was used in this experiment were the following: 50 wt. %:0 wt. %, 45 wt. %:5 wt. %, 20 wt. %:5 wt. %, 35 wt. %:15 wt. %, 15 wt. %:10 wt. %, 25 wt. %:25 wt. %, 10 wt. %:15 wt. %, 15 wt. %:35 wt. %, 5 wt. %:20 wt. %, 5 wt. %:45 wt. % and 0 wt. %:50 wt. %.


The injectability results are shown in FIG. 3.


Example 13—In Vitro Release Assay

100 to 500 mg of formulation was added to 20 to 50 ml of physiological buffer. The physiological buffer that was used was KRT containing 50 ml Krebs/Ringer/Tris (KRT) buffer pH 7.4, which is 143 mM Sodium Chloride, 5.1 mM Potassium Chloride, 2.7 mM Calcium Chloride, 1.34 mM Magnesium Sulfate, 25 mM Tris-Cl pH 7.4 and 0.1% sodium azide. Upon injection, the solvent diffused away from the formulation and the remaining polymer formed a solid biodegradable implant within the aqueous environment.


In order to maintain sink conditions, for drug release, the release medium was maintained under constant shaking at 180 rpm (Unimax 1010 apparatus, Heidolph) at 37° C. At pre-determined time intervals, media are collected and analyzed by HPLC. The amount of the GLP-1 analogue peptide M53, released from the formulation was calculated from a calibration curve. The concentration of M53 ranged between 0 and 5 mg/ml or it ranged between 0 and 200 μg/ml.


The results are shown in FIG. 4 and FIG. 5. FIG. 5 illustrates the release rate of formulations 177, 224, 225, 246 and 250 as shown in Table 1, while FIG. 4 shows the cumulative release of drug from the indicated formulations.


When the GPL-1 analogue was incorporated into the polymer solution, it was encapsulated within the polymer matrix as it solidified. The drug was then released either by diffusion inside the matrix or by biodegradation of the matrix.


Example 14—Pharmacokinetic Study

Several formulations were tested in a pharmacokinetic study in rats. Compositions containing 1 mg of drug per animal of the formulations of 177, 224, 225, 246 and 250, as set forth in Table 1 were subcutaneously administered to rats. Blood samples were collected into EDTA tubes at different time points, centrifuged and the plasma from each time point was retained. The plasma samples were analyzed by LC/MS/MS and quantified for drug content. Results are presented as ng/ml of plasma measured over time.


The results of one pharmacokinetic study are shown in FIG. 6. As shown in this Figure three of the five formulations sustain plasma concentration higher than 0.1 ng/ml for more than 28 days while giving a moderate initial drug burst release below 30 ng/ml.


Example 15—Blood Glucose Levels

Blood glucose levels with patients suffering from diabetes type 2 are taken prior to treatment. A control group having no treatment is used for this study. Patients of either gender are used in this study provided that they have diabetes type 2 and are between the ages of 35 and 60.


A GPL-1 analogue is formulated according to Examples 1 and 2 and has the chemical characteristics of number 230 in Table 1. The injectable liquid that is obtained is then injected into several patients at a dosage of 8 mg/ml. The control group is given PBS.


The amount of blood sugar levels and fructosamine is then measured for a period of 30 days, twice weekly, before meals and 2 hours after meals. The amounts of blood glucose after treatment are measured and the results are averaged. The values are shown in Table 11:













TABLE 11







Blood Glucose
Blood Glucose





Level Before
Level After


Week
Patient
Meals
Meals
Fructosamine


number
number
in mmol/l
In mmol/l
μmol



















Prior to
1
150
190
300


Treatment



2
130
175
320



3
200
230
330



4
220
240
360


1
1
90
150
280



2
98
110
290



3
120
160
330



4
215
240
365


2
1
92
120
275



2
95
100
287



3
118
158
300



4
210
230
370


3
1
92
110
270



2
98
101
275



3
115
155
280



4
211
222
385


4
1
93
110
260



2
85
100
260



3
110
150
265



4
223
244
365









Normal results for the glucose levels before meals range from 80 to 120 mmol/l. Normal results for the glucose levels after meals should be 160 mmol/l or less. Normal fructosamine levels are under 265. Between 265 and 280 indicates excellent blood glucose control; 280 and 500 indicates good blood glucose control; between 320 and 340 indicates fair blood glucose control; and over 350 indicates poor blood glucose control.


Patient 4 was administered the placebo.


These results show that when administered the biodegradable drug delivery compositions of the present invention are effective to treat diabetes type 2.


While the invention has been described in terms of various preferred embodiments, the skilled artisan will appreciate that various modifications, substitutions, omissions and changes may be made without departing from the scope thereof. Accordingly, it is intended that the scope of the present invention be limited by the scope of the claims, including equivalents thereof.

Claims
  • 1. A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula: Av-Bw-Ax
  • 2. The biodegradable drug delivery composition according to claim 1, wherein the at least one pharmaceutically hydrophobic active principle one of which is risperidone, ivermectin, levonorgestrel, cyclosporine, progesterone, bupivacaine base or medroxyprogesterone acetate.
  • 3. A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula: Av-Bw-Ax
  • 4. The biodegradable drug composition according to claim 3, wherein the at least one pharmaceutically hydrophobic active principle one of which is risperidone, ivermectin, levonorgestrel, cyclosporine, progesterone, bupivacaine base or medroxyprogesterone acetate.
  • 5. A biodegradable drug delivery composition comprising: (a) a biodegradable triblock copolymer having the formula: PLAv-PEGw-PLAx
  • 6. The biodegradable drug delivery composition according to claim 5, wherein the at least one pharmaceutically hydrophobic active principle one of which is risperidone, ivermectin, levonorgestrel, cyclosporine, progesterone, bupivacaine or medroxyprogesterone acetate.
CROSS REFERENCE TO RELATED APPLICATIONS

This application is a Continuation of U.S. application Ser. No. 16/049,580, filed on Jul. 30, 2018, which is a Continuation of U.S. application Ser. No. 14/410,994, filed on Dec. 23, 2014, which is the National Phase of PCT International Application No. PCT/IB2013/001547, filed on Jun. 27, 2013, which claims priority under 35 U.S.C. 119(e) to U.S. Provisional Application No. 61/665,192, filed on Jun. 27, 2012, all of which are hereby expressly incorporated by reference in their entirety into the present application.

Provisional Applications (1)
Number Date Country
61665192 Jun 2012 US
Continuations (2)
Number Date Country
Parent 16049580 Jul 2018 US
Child 16692487 US
Parent 14410994 Dec 2014 US
Child 16049580 US