Patent Grant
8226598
A large number of drugs and other medicaments are routinely prepared and administered to patients in a health care facility. Sometimes, two components of a therapeutic composition are required to be mixed immediately prior to administration. One method for mixing therapeutic compositions immediately prior to administration includes mixing two solutions in a mixing vessel, whereupon the mixture is drawn into a syringe, and the resulting mixed composition is then applied to an appropriate site of the patient. However, this process is often cumbersome, a significant amount of the drug may be lost, and the time between the mixing and the application is often too long with sensitive compositions (i.e., compositions that, upon mixing, must be immediately administered).
Another method for mixing therapeutic compositions immediately prior to administration employs two syringes that are clamped together. Output ends of the syringes are inserted into a Y-shaped coupling device having two input openings and a single output opening. Mixing occurs in the Y-shaped coupling device or in a needle connected to the single output end of the Y-shaped coupling device. However, with this type of arrangement, control over the degree of mixing does not exist and the degree of mixing, therefore, may be inadequate.
Another method for mixing therapeutic compositions immediately prior to administration includes coupling two syringes with an independent coupling means, thereby allowing the contents of one syringe to be mixed with the contents of the other coupled syringe. The independent coupling means, however, provides a space where there is very little agitation due to plug flow of the contents. The contents, therefore, do not mix well. Additionally, when the syringes are uncoupled (i.e., disengaged), the contents have to be aspirated out of the independent coupling means or they will be lost. In addition, the independent coupling means must be removed and discarded before attaching a needle to the delivery or injection syringe.
U.S. Pat. No. 4,994,029 (the '029 patent) discloses a syringe mixer and injector device formed of an injector and an adapter having opposed interconnectable nozzles on their facing ends and sockets and a short tubular spike in each socket to penetrate the stopper of a vial when connected to that socket. See, the '029 patent col. 2, 11. 24-31. It is among the additional objects of the invention to provide such a device which can be used with a receiving vial charged with a medicament solid or liquid, and a charging vial charged with a medicament liquid for one-way transfer to the receiving vial for admixing the medicaments therein without retransfer to the charging vial. Id. at col. 2, 11. 38-24 and col. 6, 11. 23-30. The injector inner end has a connection, provided with a nozzle recess containing a tapered, e.g. central, spout defining the inner terminus of pathway 5 and a lock connection formation, such as a luer lock tab, arranged to form a male connection formation for interconnecting releasably with mating parts on adapter 30. Col. 4, 11. 5-12. Since the '029 patent explicitly discloses that the system is made for one-way transfer, without recharging the charging vial, it would not be suitable for the recombination of materials between two syringes.
Since the system disclosed in the '029 patent was not contemplated for multiple-pass use (i.e., recombination of materials between two syringes), the skilled artisan would not use the '029 patent disclosure for a syringe system wherein multiple-pass use is desired. This is so because a system not contemplated for multiple-pass use, that is nonetheless employed for multiple-pass use, can result in an appreciable amount of sample loss (e.g., leakage). This is especially troublesome when the drug is expensive (e.g. leuprolide acetate). This is also troublesome since the U.S. Food and Drug Administration (FDA) requires that the health care professionals administer an active ingredient in a precise and known amount. Obviously, this requirement cannot be met when there is an appreciable amount of sample loss due to the syringe assembly.
U.S. Pat. No. 6,223,786 (the '786 patent) is directed to devices and methods for mixing medication and filling an ampule of a needle-less injector prior to an injection, which includes a reagent holder and a diluent holder. See, the '786 patent, col. 2, 11. 6-15. The diluent holder includes a plunger which is depressed to load the diluent from the diluent holder into the reagent holder to mix with the reagent to produce a liquid medication for filling the ampule of the needle-less injector. Id. at col. 2, 11. 20-25. In further embodiments, the reagent holder further includes a reagent plunger rod. Id. at col. 2, 11. 24-26. There is no disclosure or suggestion either explicitly or implicitly to include a male or female end forming a fluid tight engagement. In fact, the only engagement disclosed is a thread like engagement without any mention to fluid tightness. Moreover, the engagement disclosed by the '786 cannot be locked, as the threaded engagement has no means of locking.
In the most simplistic embodiment, the '786 patent discloses a four part system: diluent holder, support brushing, reagent holder, and the needleless injector; while the '029 patent discloses a four part system: injector, plunger vial, adaptor and charging vial. The presence of multiple (e.g., four) components increases the likelihood of human error when mixing and administering a drug. Additionally, the presence of multiple components increases the likelihood of an occurrence of sample loss (e.g., leakage).
Thus, there is a need for a syringe system wherein components of a composition can be easily mixed by the end user without losing a significant amount of mixed composition during the mixing process and wherein the mixed composition can be easily and rapidly administered to a patient. Such a syringe system will have a relatively few number of interconnecting parts, to minimize human error and to minimize sample loss. Additionally, the syringe system will effectively mix the contents located therein without sample loss, such that it will be approved by the FDA when used with drugs that must be administered in a known, discrete and precise amount (e.g., leuprolide acetate).
The present invention provides a syringe system wherein components of a composition can be easily mixed by the end user without losing a significant amount of mixed composition during the mixing process and wherein the mixed composition can be easily and rapidly administered to a patient. The syringe system has a relatively few number of interconnecting parts, to minimize human error and to minimize sample loss. Additionally, the syringe system effectively mixes the contents located therein without sample loss, such that it can be approved by the FDA when used with drugs that must be administered in a known, discrete and precise amount (e.g., leuprolide acetate).
The present invention provides a coupling syringe system for obtaining a mixed composition, a method for forming a mixed composition that employs such a coupling syringe system, and a method for administering a mixed composition to a patient, that employs such a coupling syringe system.
The coupling syringe system includes a first syringe, a first syringe plunger, a second syringe, and a second syringe plunger. The first syringe includes a first syringe barrel having a first syringe open proximal end and a first syringe distal end. The first syringe further includes a first syringe tip with a male end portion, wherein the male end portion has a locking ring and a tip. The first syringe barrel has a first syringe inner surface. The first syringe plunger is slidably disposed within the first syringe barrel. The first syringe plunger is in fluid-tight engagement with the first syringe inner surface. The second syringe includes a second syringe barrel having a second syringe open proximal end and a second syringe distal end. The second syringe further includes a second syringe tip with a female end portion, wherein the female end portion includes one or more exteriorly protruding members adapted to detachably fit the locking ring. The second syringe barrel has a second syringe inner surface. The second syringe plunger is slidably disposed within the second syringe barrel. The second syringe plunger is in fluid-tight engagement with the second syringe inner surface. The female end portion has an opening therein. The opening is sized and configured to receive the tip of the male end portion therein. The locking ring couples the first syringe to the second syringe when the tip of the male end portion is disposed within the female end portion, forming a fluid tight engagement.
The coupling syringe system of the present invention allows for the effective mixing of compositions immediately prior to administration. The mixing does not result in a significant loss of the composition. In addition, the time between the mixing and the administration of the composition is minimal, such that a sensitive composition (i.e., a composition that, upon mixing, must be immediately administered) is not chemically or physically altered (i.e., there is minimal decomposition). The use of the coupling syringe system of the invention does not result in a plug flow of the contents. In addition, the coupling syringe system can conveniently be disassembled and a needle can conveniently be attached to the syringe which includes a male end portion and a locking ring.
Referring to
The locking ring 11 is configured such that the interior of the locking ring 11 contains threads which are adapted to receive protruding members 12 exteriorly disposed on the female end portion of the second syringe 14 as shown in
As shown in
As shown in
As shown in
As shown in
As shown in
In an alternative embodiment, a first securing device can conveniently be mounted on the interior surface of barrel 2 or on the inside of barrel 18. The first securing device, upon engaging with a second securing device mounted on the external surface of plunger 40 or plunger 90, respectively, can prohibit the plunger 40 or the plunger 90 from disengaging from barrel 2 or the barrel 18, respectively.
The first syringe and the second syringe can conveniently be manufactured from any suitable material. Typically, both the first syringe and the second syringe are each independently manufactured from glass or plastic (e.g., polypropylene, polyethylene, polycarbonate, polystyrene, and the like).
The size of both the first syringe and second syringe can independently be any suitable size. Suitable sizes include a syringe barrel of about 0.01 to about 100 cc, about 0.1 cc to about 50 cc, about 0.1 cc to about 25 cc, or about 0.5 cc to about 10 cc.
The first syringe 13 (i.e., the syringe including the male end portion and locking ring) can conveniently be manufactured by any suitable process. The first syringe can conveniently be manufactured by an injecting molding process where the entire syringe is made as one unit. Alternatively, the first syringe can be manufactured by independently molding the syringe and locking ring and then mounting (i.e., attaching) the locking ring and first syringe. Preferably, the locking ring is permanently attached to the first syringe. Although the ring can also be mounted coaxially and rotably with tip 8 by a flange and seal configuration. In this configuration, the ring can be rotated around the tip. Typically, the locking ring is permanently attached to the first syringe by welding the two pieces together.
The second syringe 14 (i.e., the syringe including the female end portion) can conveniently be manufactured by any suitable process. The second syringe can be manufactured by an injecting molding process where the entire syringe is made as one unit.
Each composition to be combined with a syringe can independently be a solid, liquid, or mixture thereof. In addition, the solid can be a powder or crystalline material. As used herein, a mixture of a solid and a liquid can be a heterogeneous phase (e.g., an emulsion or a colloidal suspension). Alternatively, a mixture of a solid and a liquid can be a homogeneous phase (i.e., a solid completely dissolved in a liquid).
Each composition can independently include one or more (e.g., 1, 2, or 3) compounds. In addition, the compound of the composition can be a drug delivery system, a drug (i.e., pharmaceutical) or a pharmaceutically acceptable salt thereof, a liquid carrier, a liquid, a lipid formulation, or a vaccine.
Any suitable drug delivery system can be employed. A suitable drug delivery system includes, but is not limited to, is the Atrigel® delivery system mixed with doxycycline or leuprolide acetate. The Atrigel® system is described in U.S. Pat. No. 5,278,201, the disclosure of which is incorporated herein by reference.
Any suitable drug (i.e., pharmaceutical) or pharmaceutically acceptable salt thereof can be employed. Suitable classes of drugs include antibiotics, peptides, hormones, analgesics, growth factors, and any agent described in U.S. Pat. No. 4,938,763B1, the disclosure of which is incorporated herein by reference. The drug can exist as a solid (e.g., crystal or powder), an oil, or as a liquid. In addition, the drug may exist in a microcapsule containing the drug or as a microparticle.
Any suitable liquid carrier can be employed. Suitable liquid carriers include a collagen solution, a sterile aqueous solution, a sterile saline solution, an alcoholic solution, or any suitable mixture thereof. In addition, the liquid carrier can be an emulsion formed from a mixture of an oil or lipid with a sterile aqueous solution or a sterile saline solution.
Specifically, the liquid drug delivery system can be the Atrigel® system mixed with a powder drug (e.g., doxycycline or leuprolide acetate).
Specifically, the drug can be an antibiotic or growth factor.
Specifically, the liquid carrier can be a collagen solution and a powder drug.
Specifically, the liquid carrier can be a sterile aqueous or a sterile saline solution and a powder drug.
Specifically, the liquid can be an alcohol and a drug mixed with a sterile saline or a sterile aqueous solution.
Specifically, the lipid formulation can be mixed with a sterile aqueous solution or a sterile saline solution to form an emulsion.
Specifically, the liquid carrier (e.g., a sterile aqueous solution or a sterile saline solution) can be mixed with a microcapsule or a microparticle containing drug.
Specifically, the vaccine solution can be mixed with an oil to form an emulsion.
Any suitable method of administration can be employed. Typically, the mixed composition can be administered to a patient by intravenous, intramuscular, intraperitoneal, or subcutaneous routes.
Both the amount of drug and the drug content, delivered from a syringe system of the present invention, is relatively uniform. Additionally, there is relatively low sample loss when delivering a drug from syringe system of the present invention.
The LA-2575 30.0 mg drug product when injected subcutaneously forms a biodegradable implant that delivers 30.0 mg of leuprolide acetate (LA) over a four-month period. The drug product is composed of two separate syringes. Syringe A with a female Luer Lok fitting contains the drug delivery vehicle, and Syringe B with a male Luer Lok fitting contains lyophilized LA. To constitute the product for injection, Syringe A and Syringe B are connected, and the contents are passed back and forth until blended. After mixing, the two syringes are separated, a hypodermic needle is attached to Syringe B, and the constituted drug product is administered subcutaneously to the patient.
A fraction of the constituted drug product is trapped in the hub of Syringe A after the mixing process and in the hub and needle of Syringe B after injection. To meet the targeted delivery values, this retained drug product must be accounted for when calculating the fill weights for both syringes. Also, the amount of material and drug delivered from the mixed syringe must be consistent in quantity to meet strict FDA rules for administered drug. To determine whether the amount of material and drug administered was consistent, an experiment was performed with the following supplies:
Each of three lab analysts constituted 10 replicate units using 30 mixing cycles and determined delivered mass and % LA content. The data given in the table show that the delivered mass was consistent with a delivered mass of 504.4±6.55 mg and the mixing was uniform with a drug content of 5.6±0.19%. These data show that the syringe coupling system gives uniform mixing of the contents and reproducible delivery of the mixed mass.
The 6-Month ELIGARD 45.0 mg drug product when injected subcutaneously forms a biodegradable implant that delivers 45.0 mg of leuprolide acetate (LA) over a six-month period. The drug product is composed of two separate syringes. Syringe A with a female Luer Lok fitting contains the drug delivery vehicle, and Syringe B with a male Luer Lok fitting contains lyophilized LA. To constitute the product for injection, Syringe A and Syringe B are connected, and the contents are passed back and forth until blended. After mixing, the two syringes are separated, a hypodermic needle is attached to Syringe B, and the constituted drug product is administered subcutaneously to the patient.
A fraction of the constituted drug product is trapped in the hub of Syringe A after the mixing process and in the hub and needle of Syringe B after injection. To meet the targeted delivery values, this retained drug product must be accounted for when calculating the fill weights for both syringes. An experiment was conducted to determine the amount of total mass delivered, the amount of drug, and the drug content when the two syringes were mixed. The following supplies were used in this experiment:
Each of three lab analysts constituted six replicate units using 60 mixing cycles and determined delivered mass and % LA content. The results given in the table show that the delivered mass was consistent with 371.4±4.5 mg, the amount of drug delivered at 45.5±0.8 mg, and the drug content at 12.3±0.2%. These data show that the unique syringe coupling system gives both uniform mixing of the contents and reproducible delivery of the mixed mass.
This application is a continuation-in-part of U.S. patent application Ser. No. 09/405,463, filed Sep. 24, 1999, now abandoned, which application is incorporated herein by reference.
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| Number | Date | Country | |
|---|---|---|---|
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| Number | Date | Country | |
|---|---|---|---|
| Parent | 09405463 | Sep 1999 | US |
| Child | 10634656 | US |
