The present invention relates to subcutaneous implants obtained by extrusion containing an active ingredient, and a hydrophilic excipient dispersed in a PLGA matrix.
Many active ingredients are rapidly metabolized and eliminated by the human or mammalian organism, therefore requiring frequent administration of the drug with the aim of maintaining an adequate therapeutic concentration.
An example of controlled release implants are represented by subcutaneous implants.
Among the numerous implants previously described, the subcutaneous implants described in WO00/33809 represent a net improvement with reference to previous subcutaneous implants containing as the active principle a polypeptide dispersed in a matrix of polylactic-glycolic acid in that they are able to release the aforesaid active principle in 6 months. The subcutaneous implants described in said previous patent differ also in that they present an essentially triphasic and not biphasic release profile as clarified in the following manner: release by pure diffusion, diffusion by release following to swelling and release by polymer degradation.
This progression therefore allows for an extension of release times. In fact when these implants are introduced into an aqueous medium, the water diffuses through the polymeric matrix reaching the peptide particles closest to the surface and subsequently the inner zones.
The implant remains substantially unmodified for about 6 weeks and in this period releases approximately 30% of the peptide.
The duration of this stage of pure diffusion is essentially determined by the level of heterogeneity of the peptide dimensions and the rate is essentially determined by the particle content in the PLGA matrix.
As the active principle presents heterogeneous dimensions, a sufficient quantity of peptide remains after the first stage of dissolution and can be released in the successive stages mentioned, that is release by diffusion and swelling, or release by disintegration of the polymer.
Subcutaneous implants including those above described suffer from a drawback essentially caused by the fact that the active ingredient release rate during the three successive phases is partially governed by the concentration of active ingredient within the polymeric matrix (the other factors being the intrinsic solubility and diffusion properties of the active ingredient and the characteristics of the PLGA). On one hand, the amount of active ingredients (dose) to be incorporated into the implant depends on the activity of the product and on the expected dosing interval. However big dimensions implants create problem insofar patients compliance is concerned on the other hand small dimensions subcutaneous implants create problems under industrial feasibility aspects since a very thin or very short implant may be difficult to handle and to package.
It may therefore happen that implants containing a small amount of very potent active ingredient within a “normal” size (i.e. around 1 mm diameter and 1 cm length) presents a very low active ingredient concentration within the polymeric matrix, thus leading to a poor release profile especially in the first two weeks from the administration, afterwards a marked and abrupt release resulting in an overall shortened period if compared to subcutaneous implants containing higher amounts of the active ingredient.
The Applicant has now unexpectedly found subcutaneous PLGA based implants formulations which overcome the above drawback.
The present invention therefore relates to subcutaneous implants composed of a PLGA based polymeric matrix containing dispersed therein an active ingredient and a hydrophilic excipient so that the weight ratio:
(Active Ingredient (AI)+Excipient (E))/PLGA is higher than 0.05 and lower than 1.
In fact the subcutaneous having said weight ratio lower than 0.05 behave like the aforesaid subcutaneous implants containing a low amount of active ingredient in the absence of hydrophilic excipient, namely they exhibit a poor release profile especially in the first two weeks from the administration, afterwards a marked and abrupt release resulting in an overall shortened period if compared to subcutaneous implants containing higher amounts of the active ingredient, whereas the subcutaneous implants having the aforesaid weight ratio equal to or higher than 1, release too quickly the active ingredient.
On the contrary the implants of the invention result to release the active ingredient therein contained with the typical triphasic profile and the presence of this excipient within the formulation modify the release rates during the three successive phases and also modify the overall release duration.
The aforesaid weight ratio is preferably comprised between 0.3 and 0.9, more preferably between 0.4 and 0.8.
The hydrophilic excipient is preferably selected from mannitol, sorbitol, trehalose, polyvinylpyrrolidone having an average molecular weight ranging from 6000 to 10000 Da more preferably 8000 Da.
The subcutaneous implants of the present invention preferably contain an active principle chosen from the class consisting of: a peptide, an analgesic-narcotic active principle.
More preferably said peptide is chosen from: avorelin, triptorelin, goserelin and leuprorelin.
As “drugs with narcotic analgesic activity” preferred are morphine and morphinans, i.e. compounds having a chemical structure and activity similar to that of morphine i.e. μ receptor agonists, but also compounds with morphinic-type activity, in other words also μ receptor agonists but with a different chemical structure such as those belonging to the phenylpiperidine class. (Goodman & Gilman's “The pharmacological basis of therapeutics” Ninth Edition Chapter 23 pages 521-555).
As phenylpiperidine μ receptor agonists we cite as preferred at least one active principle chosen from the class consisting of meperidine, fentanyl and relative pharmaceutically acceptable salts, fentanyl congeners, for example sufentanyl, alfentanyl, lofentanyl, carfentanyl, remifentanyl and their pharmaceutically acceptable salts.
Preferably, when the subcutaneous implants according to the present invention contain a peptide as the active ingredient, they show a heterogeneous particles size distribution more preferably ranging from 1 to 63 μm or from 1 to 100 μm.
Specifically, when the subcutaneous implants of the invention contain the peptides having the aforesaid heterogeneous particles size dimensions, also the hydrophilic excipient has heterogeneous particles size distribution preferably ranging from 10 to 250 μm.
When the hydrophilic excipient is mannitol it is preferably present in the subcutaneous implants in weight ratio with respect to the active ingredient in amounts ranging from 2:1 to 5:1 and more preferably in weight ratio of 4:1.
When the hydrophilic excipient is trehalose or polyvinylpyrrolidone it is preferably present in weight ratio with respect to the active ingredient in amounts ranging from 1:6 to 1:1, more preferably of from 1:5 to 1:2.
The PLGA contained in the subcutaneous implants according to the present invention has preferably a weight average molecular weight of from 50000. to 150000 Da and a lactic acid/glycolic acid ranging from 50/50 to 95/5.
As PLGA polymeric matrix the subcutaneous implants according to the present invention may contain a sole PLGA or that obtained by grinding an extruded product of a blend of:
The present invention further relates to
We report herewith for illustrative but not limiting purposes an example of preparation of subcutaneous implants according to the present invention.
Subcutaneous implants containing ingredients as described in the table below are prepared as described in WO00/33809
It is observed that the typical triphasic release pattern and a 3 months release duration are obtained with 25.0% w/w loading of active agent (Form. 1#1). On the contrary neither the profile nor the duration is maintained when loading the matrix at 5.0% w/w (Form. 1#3). Finally the triphasic profile and the 3 months duration are recovered when adding 20.0% w/w of mannitol to the 5.0% w/w of active agent (1#2).
In the case of the low active ingredient loading ((AI+E)/PLGA ratio=1/19), a very limited number of channels exists within the polymeric matrix. The degradation of the polymeric matrix through autocatalysis is therefore accelerated (this leading to a shorter overall release duration). When adding 20% of a very hydrophilic small molecule (Mannitol), a lot of channels are opened so that the circulation of dissolution buffer within the matrix is sufficient to limit the autocatalysis process and, as a consequence, the release of active ingredient are higher in the first weeks than with subcutaneous implants containing the same amount of active ingredient in the sole PLGA and contemporaneously the matrix resists for longer time to hydrolysis.
Subcutaneous implants containing ingredients as described in the table below are prepared as described in WO00/33809
A 40 mg implant according to formulation 2#1 contains 11.6 mg of Active ingredient when, according to formulations 2#2 and 2#3, the same implant contains 8 mg of active ingredient.
It is observed that both formulations 2#1 and 2#2 present the typical triphasic release pattern and a 3 months long release duration. With a similar (≈2/5) AI+E/PLGA ratio, these two formulations operate properly even if it is also noticed in this case that the presence of a small hydrophilic molecule (trehalose) tends to increase the dissolution rate during the first month and to delay the second burst (PLGA degradation driven).
The dissolution profile from formulation 2#3 is also very informative. In this case, AI+E/PLGA ratio is close to 1/1. This means that half of the matrix is occupied by very hydrophilic molecules. Once dropped into the dissolution medium, such an implant presents a huge number of channels allowing the active ingredient to leave the matrix (through a percolation process).
It is interesting to notice that formulation 2#1 (containing 11.6 mg of active ingredient per depot) and formulation 2#2 (containing 8.0 mg of active ingredient per depot) release almost the same amount of active ingredient over the entire first month after immersion.
The use of an excipient is clearly a powerful formulation tool. It is useful to allow for a specific implant to operate properly even with low active ingredient loading but it is also useful to modulate a suboptimal release profile up to exactly reach the target
Subcutaneous implants containing ingredients as described in the table below are prepared as described in WO00/33809
It is also observed that, in this case, polyvinyl pyrrolidone (PVP) appears to show better hydrophilicity if compared to Mannitol added at the same weight as PVP
Number | Date | Country | Kind |
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MI2006A001539 | Aug 2006 | IT | national |
Filing Document | Filing Date | Country | Kind | 371c Date |
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PCT/EP2007/057961 | 8/1/2007 | WO | 00 | 1/28/2009 |