“Not Applicable”
“Not Applicable”
“Not Applicable”
This invention relates generally to container capping systems and more particularly to systems and methods for capping pharmaceutical vials.
For more than sixty years injectable drugs have been packed in glass vials. Such vials typically are formed of glass and have a cylindrical neck terminating in a flanged top or lip, with the opening to the interior of the vial extending through the neck. The neck is sealed by means of a rubber stopper and an aluminum seal or ferrule. When these types of vials are used in lyophilization (freeze drying) the vial is filled with liquid and then the stopper (which is a complex or complicated elastomeric member) is inserted part way into the vial so that the product can be lyophilized. In this regard, the standard stopper and vial combination often rely on a feature called a “blowback” on the inside of the vial's lip to mate with an indentation on the elastomeric stopper. This action keeps the stoppers from rising up during processing. Once the lyophilization process has occurred the stopper is then fully seated in place, e.g., pushed down, so that it is completely within the neck of the vial during the final stages of the process and a ferrule applied to lock the stopper in place to thereby permanently seal the vial. Needless to say this is a complex operation and requires that the entire operation be accomplished within sterile conditions, e.g., within the freeze drying apparatus. Moreover, the construction of the closures require the use of vials having the blowback feature, thereby limiting the materials that can be used to form the vials to glass, e.g., plastic materials have not proved economically viable for producing vials with a viable blowback feature.
Accordingly, a need exists for a capping system, particularly one that is suitable for lyophilization applications, which overcomes the drawbacks of the prior art.
The subject invention addresses that need.
In accordance with one aspect of the invention there is provided a cap system for sealing a pharmaceutical vial having an opening to the interior of the vial and a flanged neck surrounding the opening, the flanged neck having an undersurface. The cap system comprises a closure assembly (e.g., a pre-assembled unit) having an elastomeric stopper and a retainer member. The elastomeric stopper has a body portion. The retainer member includes a top wall and a peripheral sidewall. The sidewall comprises plural resilient fingers that are located about the periphery of the sidewall. The stopper is arranged to be secured to the vial so that the body portion of the stopper partially closes the opening of the vial. The retaining member is arranged to be secured to the vial with its fingers arranged to flex over the flanged neck of the vial and then to snap into engagement with the undersurface of the flanged neck of the vial. Portions of the top wall of said retainer member are then in engagement with portions of the stopper to hold the stopper in place (e.g., slightly compress the stopper) on the vial to seal the opening in the vial.
In accordance with one aspect of this invention the vials using the closure of the foregoing cap system can be readily used for in-vial lyophilization of pharmaceuticals within a freeze drying apparatus to temporarily seal the contents within the vial. The then the closures on the vials can be permanently sealed (i.e., the temporary seal locked) by means of a locking member, also forming an aspect of this invention. The locking member can be applied at any other location, even a non-sterile location.
In accordance with another aspect of this invention method for capping plural pharmaceutical vials is provided. Each vial includes an interior in which a lyophilizable material is located, with the vial having an opening to the interior of the vial and a flanged neck surrounding the opening. The flanged neck has an undersurface. The method basically entails providing a plurality of such pharmaceutical vials in a tray. Each vial is provided with a respective closure assembly comprising an elastomeric stopper and a retainer member on the neck of its associated vial so that a portion of the stopper partially closes, but does not seal, the opening of the vial (e.g., moisture can pass through a gap or interface between the stopper and the immediately adjacent portion of the neck of the vial). A waterproof/breathable fabric membrane, e.g., Gore-tex® fabric, cover is disposed over the vials within the tray to enclose the vials with their respective closure assemblies within the tray and the tray with the vials and cover is placed in a freeze drying chamber to lyophilize the contents of the vials, whereupon the moisture extracted from within the vials passes through the membrane cover out of the tray (e.g., moisture passes through the interface between the stopper and neck of the vial and through a communicating slot in the retainer member). A force can then be applied to the closures within tray after the contents of the vials have been lyophilized to cause the retainer member to snap-fit on the flanged neck of the associated vial so that portions of the associated stopper seal the opening in the associated vial (e.g., a fluid-tight fit is produced at the interface of the stopper and the neck of the vial).
The tray with the sealed lyophilized vials can then be removed from the freeze drying chamber for further processing, if desired. To that end, and in accordance with another method aspect of this invention after the tray with the sealed lyophilized vials has been removed, the vials can be removed from the tray or left in the tray but taken to a different location for further processing. That further processing can consist of securing a locking member over the closures to form a permanent seal for the vials.
Referring now to the various figures of the drawing wherein like reference characters refer to like parts, there is shown in
The closure assembly 22 or the entire capping system 20 of this invention are particularly suitable for use on pharmaceuticals vial, such as a glass vial 2 used for injectable drugs, but owing to the construction of the closure assembly it/they can also be used on vials made of plastic. Before describing the details of the closure assembly 22 and the locking cap member 28 a brief description of the vial on which they can be used is in order. To that end, as best seen in
The details of the inner closure assembly 22 will now be described. To that end, as can be seen best in
The retainer member 26 is of a general cup-like shape and can be formed of any suitable plastic material, e.g., polypropylene, that is sufficiently strong, yet having some flexibility (for reasons which will be apparent later). The retaining member 26 can be molded as an integral unit and basically comprises a top wall 26A and a peripheral sidewall 26B. The center portion of the top wall is open at 26C to provide access to the stopper so that a needle or other piercing device can be inserted therethrough. The peripheral sidewall 26B includes a plurality of slots 26D equidistantly spaced from one another. The portions of the sidewalls between the slots 26D form respective, downwardly extending flexible talons or fingers 26E. As best seen in
That operation is best seen in
As will be appreciated by those skilled in the art, the foregoing operation is suitable for sealing vials with liquid drugs under sterile conditions. For applications in which the drug is to be lyophilized (freeze-dried), a plurality of filled vials 2 can be provided with respective closure assemblies 22 and placed within a specially constructed pre-sterilized tray assembly 100 in a sterile freeze drying chamber. The vials are filled in rows without leaving the trays.
Once the upper tray with the preassembled closure assemblies has been placed in the lower tray so that each vial in the array has a respective closure assembly disposed immediately above it, a moisture permeable (e.g., waterproof/breathable) membrane 122, e.g., a sheet of Gore-tex® membrane, is disposed over the tray and secured, e.g., heat sealed, to the flange 106 of the lower tray as best seen in
Since the closure assembly 22 of this invention compresses the elastomeric stopper 24, the sealed vials can be moved out of sterile conditions (European grade A or U.S. class 100) for additional processing steps and the application of an outer security seal, e.g., a locking cap member 28 (which will be described shortly). Thus, the closure assembly of this invention allows a manufacturer to utilize tray filling and processing of injectable drugs. In this process, pre-sterilized vials are provided to the filling company in trays.
The closure assemblies of this invention can be used in various ways. For example, they can be sold in bulk to a company that is filling liquids. In such a case the closure assemblies would be applied to vials as they now apply just the stopper to vials. The advantage of the closure assemblies of this invention for that application is that the stopper is compressed and the package is secure at the stoppering station, which does not now occur with the prior art. A second way that closure assemblies of this invention can be used is to provide them in bulk to a company that would use them in freeze drying. In such an application the closure assemblies would be inserted into the vials into the “up” position (the position shown in
As mentioned earlier the standard prior art stopper and vial combinations often rely on a feature called a blowback on the inside of the lip of the glass finish of the vial to mate with an indentation on the elastomeric stopper to keep the stoppered vials from raising up during processing. Since the closure assembly of this invention locks on to the outside of the neck of the vial, the blowback feature of the prior art can be eliminated. Moreover the manner in which the closure assembly of the subject invention locks to the outside of the vial provides a security benefit when using vials manufactured from thermoplastic materials that cannot include a blowback feature.
While the seal produced by the operation of the closure assembly of this invention is suitable for keeping the contents of the vial sterile for at least short period of time, for many applications a more permanent seal would be deemed necessary. In such a case the locking cap member 28 forming another part of the capping system of this invention is used to permanently lock the closure assembly in place on the vial. This process will best be understood by reference to
In the interest of brevity the details of the closure assembly 22 will not be reiterated. Turning now to
The locking cap member 28 is disposed on the top of the retainer member 26 so that the undersurface of each of the lugs 28D abuts a respective portion of the top wall 26A of the retaining member as shown in
As should be appreciated from the foregoing the system of this invention is unique in that it includes an elastomeric element pre-inserted into it. This element can either be a molded stopper, where a customer wants to work with an already approved formulation that has been filed with the regulatory agencies. In fact, the elastomeric stopper can be simplified to a flat disc that is either molded or punched directly out of sheeting material. When used on liquid filled products, the inner sterility seal would be applied in one step with the sterile filling suite. When working with a material that will be lyophilized, the inner seal would be applied halfway and locked into position to be transported to the freeze drier.
Moreover, the system of this invention should prove of immense value to the pharmaceutical industry for filling vials and syringe cartridges in trays. With the elastomer inserted into it, it can be assembled into the lid of a tray to mate with vials or cartridges nested in the bottom half of the tray. In this application the entire tray would be sealed at one time keeping all of the containers intact in one tray. This same technique can be used with vials that will be lyophilized. In this case, the tray itself can be manufactured with a side panel that includes a permeable, e.g., Gore-tee membrane, section instead of using a membrane cover sheet such as described with reference to
Another feature of the system of this invention is that it enables one to provide clear evidence of tampering. In particular, the outer locking cap 28 may be formed to be clear or translucent or have a portion or window that is clear or translucent so that a lot number or other identification can be etched or printed on the retainer member 24 of the inner closure assembly 22. Thus, the lot number or other identification indicia can be read through the seal, but not be able to be altered in any way.
The closure assembly forming the inner seal of this invention can also be used with other manufacturer's devices. For example, the BD Monovial could be modified so that it could be used as the outer locking seal and applied in a final packaging area. This could also apply to other needle-less access systems or other docking devices.
Since the elastomeric stopper element 24 of this invention is housed in a plastic closure (i.e., the retaining member 26), lubricants such as silicone that have been required heretofore to track stoppers may be eliminated.
It should also be pointed out that the subject invention can be used for liquid fills, as well as freeze dried applications, allowing the closed container to leave a sterile environment with proven seal integrity and be handled in a non-classified environment. It could be made available in various finish sizes and the outer locking seal could be designed to fit with a variety of devices for administration.
Without further elaboration the foregoing will so fully illustrate our invention that others may, by applying current or future knowledge, adopt the same for use under various conditions of service.
Number | Name | Date | Kind |
---|---|---|---|
5314084 | Folta et al. | May 1994 | A |
5429256 | Kestenbaum | Jul 1995 | A |
5718348 | Manera | Feb 1998 | A |
5819964 | Grimard | Oct 1998 | A |
20070272648 | Hamamoto et al. | Nov 2007 | A1 |
20100089862 | Schmitt | Apr 2010 | A1 |
20100224632 | Aneas | Sep 2010 | A1 |
Number | Date | Country |
---|---|---|
0909719 | Apr 1999 | EP |
Entry |
---|
International Search Report for PCT/US2012/030513 mailed Jun. 27, 2012. |
Number | Date | Country | |
---|---|---|---|
20120248057 A1 | Oct 2012 | US |