Lyophilization apparatus and methods

Description

BACKGROUND OF THE INVENTION

1. Field of the Invention

The invention relates to lyophilization, more particularly to improved methods and apparatus for bulk lyophilization.

2. Description of Related Art

Freeze drying, or lyophilization, is a dehydration technique. It takes place while a product is in a frozen state (ice sublimation under a vacuum) and under a vacuum (drying by gentle heating). These conditions stabilize the product, and minimize oxidation and other degradative processes. The conditions of freeze drying permit running the process at low temperatures, therefore, thermally labile products can be preserved. Freeze drying has become an accepted method of processing heat sensitive products that require long term storage at temperatures above freezing.

Steps in freeze drying include pretreatment, freezing, primary drying and secondary drying. Pretreatment includes any method of treating the product prior to freezing. This may include concentrating the product, formulation revision (i.e., addition of components to increase stability and/or improve processing), decreasing a high vapor pressure solvent or increasing the surface area. Methods of pretreatment include: freeze concentration, solution phase concentration, and formulating specifically to preserve product appearance or to provide lyoprotection for reactive products. The term “lyoprotection” refers to stabilization during all of the freeze drying process (i.e., during both freezing and drying).

The second step is to freeze the product. Freezing the product decreases chemical activity by decreasing molecular movement. Freezing is essentially the dehydration step in freeze drying; once the solvent matrix is in the solid (frozen) state, the solute matrix is “dry,” (although it may contain some bound water. A rule of thumb for freezing product is that the product container should preferably not be filled with product to more than half of its total volumetric rating. In practice this may also mean filling the product only to certain depth to facilitate freezing, ice sublimation and final water/solvent removal. This helps insure, in most cases, that the surface to depth ratio is such that freeze drying is not impeded by the product depth.

How a product is frozen is determined in part by the type of product container and freeze dryer to be used. If larger flasks are to be used in conjunction with a manifold freeze dryer the product should be shell frozen. The rotation of a flask, around its vertical or tilted axis, either by hand in a dry ice alcohol bath or by using a bath specifically designed for shell freezing, increases the surface area substantially. This shell freezing technique promotes conditions of more compact development of large drying surfaces when freeze drying larger volumes of product in flasks although the formation of ice crystals may depend on false movement.

If large numbers of smaller product containers are to be processed in a tray dryer, static or plug freezing is performed. The serum bottle, vial or ampule is filled to the appropriate level and the product is frozen while the container is in an upright position. This type of freezing is typically employed with product volumes of 25 ml or less.

When a product is to be processed in a tray/shelf dryer, the product containers are loaded into trays for introduction to the freeze dryer. If the product has been prefrozen the shelves of the tray dryer should be pre-cooled to a temperature slightly below the freezing point of the product. In most cases the room temperature product is introduced to room temperature shelves of the tray/shelf dryer. The tray/shelf dryer refrigerator is then activated to freeze the product. The refrigerator may be used to reach the temperature below the eutectic and glassy state temperatures of product and solutes. Then the primary drying may begin, e.g. the sublimation of ice crystals at low pressure and at temperatures low enough to reduce cake softening and collapse. After removal of the ice crystals by sublimation, the remaining matrix may still contain bound water/solvent that may be removed by slow heating under low pressure conditions. The drying temperature may be gradually increased as the water content in the dried matrix decreases. Any local overheating of the product matrix may cause localized product deterioration and/or collapse.

When the product reaches a temperature above 0° C., secondary drying may have already begun. A product in secondary drying often appears dry. However, some “bound” solvent may still remain in the apparently dry product. During secondary drying, a vacuum pump creates a low pressure condition that promotes removal of bound solvents. The amount of residual water or solvent in the lyophilized product is dependent on the length of time the product remains in secondary drying. Final level of water/solvent content is important for product storage, e.g. if the water content is too high the product matrix may experience melting and collapse if the storage temperature is increased. Uniformity of water/solvent removal across large areas and volumes of product is thus very important to protect product from local deterioration during lyophilized product storage at ambient temperatures.

Once the product is at the end of its lyophilization cycle it should be removed from the freeze dryer. In a stoppering shelf/tray dryer, an inert gas may be bled into the chamber forming an inert “gas cap” over the product prior to stoppering. Many products are simply stoppered while under vacuum. The stoppers used most commonly on serum vials/bottles have a vacuum integrity of approximately 5 years when used in conjunction with tear off seals. Once the product is stoppered, the system is returned to atmospheric pressure and the shelves are unloaded.

Bulk trays may be used in lyophilization processes to preserve products or intermediates for further processing. Bulk trays typically contain many times the volume of product or intermediate contained in a conventional lyophilization stopped vial/bottle. Therefore, if it is necessary to store a product or intermediate for further processing through lyophilization, bulk lyophilization reduces the amount of handling of the product or intermediate as compared to lyophilizing in vials. This is a significant advantage in terms of cost and contamination.

However, bulk lyophilization has some drawbacks. If bulk trays are used in the freeze drying product, the system is brought to atmospheric pressure and the trays are then unloaded. Product processed in this way likely will absorb the water vapor with which it comes in contact. Consequently this product should be processed or stored as quickly as possible. Due to exposure of the product surface to the environment there is a possibility of contamination. Therefore, bulk lyophilization (filling the open trays, loading the open trays into lyophilizer and unloading the open trays from lyophilizer, etc.) requires a clean room environment, with attendant high cost of the room, cost of its maintenance, complex operational procedures, etc. Subsequent handling of powder (e.g., emptying the open trays with elevated edges) or powder reconstitution with liquid also requires a clean room environment. Further, flat, open, shallow trays being filled and handled create the possibility of spills.

Finally, bulk lyophilization trays preferably are flat enough to match the contours of the shelf and promote good heat transfer between the shelf and the tray. This condition may not be easy to maintain during multiple uses of trays—such trays may be too flimsy and may become warped. Warpage may lead to non-uniform lyophilization—a clear disadvantage.

There is therefore a need for improved methods and apparatus for lyophilization to address the problems noted above.

SUMMARY OF THE INVENTION

In an aspect, the invention relates to a bulk lyophilization container comprising a body portion; and an aseptic closure portion, wherein the body portion is coupled to the aseptic closure portion.

In another aspect, the invention relates to a bulk lyophilization container comprising a heat flux equalizer portion located so as to equalize a heat flux through the bulk lyophilization container.

In still another aspect, the invention relates to a method of lyophilization of a product comprising increasing uniformity of heat flux to or from the product during any freezing, primary or secondary drying operations that occur during the lyophilization.

In an aspect, the invention relates to a lyophilization stopper comprising three or more straight vent notches. The invention also relates to a lyophilization stopper comprising sealing ridges located on an outer surface of the lyophilization stopper, a lyophilization stopper comprising stopper window vents that penetrate the stopper, and a lyophilization stopper comprising shallow vents that do not penetrate the stopper.

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1A

shows an isometric elevation of a bulk lyophilization container according to the invention.

FIGS. 1B-C

show cross-sections of bulk lyophilization containers according to the invention.

FIGS. 2A-F

show cross-sections of bulk lyophilization containers according to the invention.

FIG. 2F

shows an isometric elevation of a bulk lyophilization container according to the invention.

FIGS. 3A-H

show isometric and top elevations of bulk lyophilization containers according to the invention.

FIGS. 4A-B

show isometric elevations of a bulk lyophilization container according to the invention.

FIG. 4C

shows a cross-section of a bulk lyophilization container according to the invention.

FIGS. 5A

, E, and F show isometric elevations of bulk lyophilization containers according to the invention.

FIGS. 5B-D

show cross-sections of bulk lyophilization containers according to the invention.

FIGS. 6A-F

show isometric and cross-sections of lyophilization stoppers according to the invention.

FIGS. 7A-L

show side and cross-section elevations of lyophilization stoppers according to the invention.

FIGS. 8A-E

show cross-section elevations of lyophilization stoppers according to the invention.

FIG. 8F

shows an isometric elevation of a bulk lyophilization container according to the invention.

FIGS. 9A-M

show cross-sections of seals according to the invention that are useful in aseptic sealing, particularly in aseptic sealing of bulk lyophilization containers according to the invention.

FIG. 10

shows a cross-section of a bulk lyophilization container according to the invention.

FIG. 11A

shows a cross-section of lyophilization container on a shelf lyophilizer.

FIG. 11B

shows a side elevation of lyophilization containers in a heat transfer bath.

FIGS. 12A-F

show cross-sections of bulk lyophilization containers according to the invention.

FIGS. 13A-C

show cross-sections of bulk lyophilization containers according to the invention.

FIGS. 14A-H

show cross-sections of bulk lyophilization containers according to the invention, emphasizing their sealing arrangements.

FIGS. 15A-E

show cross-sections of lyophilization containers according to the invention, emphasizing their heat flux equalizing portions.

DETAILED DESCRIPTION OF THE INVENTION

FIG. 1A

shows an isometric view of an embodiment of a bulk lyophilization container according to the invention.

FIG. 1B

shows a cross-sectional view of the embodiment. In

FIG. 1A

, body portion

102

, aseptic closure portion

104

, seal

105

, opening handle

106

, neck

108

, and stopper

110

are indicated. Body portion

102

is covered by aseptic closure portion

104

and sealed along seal

105

, forming an aseptic container for the product undergoing lyophilization. The use of aseptic closure portion

104

may reduce risk of contamination or spillage during tray filling with liquid and bulk lyophilization and subsequent tray handling. Additionally, use of aseptic closure portion

104

enables the inventive bulk lyophilization container to be made stiffer, with less consequent warpage during use. This may lead to improved heat transfer and thus improved lyophilization results. Therefore, inclusion of aseptic closure portion

104

in the inventive bulk lyophilization container represents a significant advance over previous attempts to perform bulk lyophilization. Opening handle

106

, coupled to aseptic closure portion

104

, enables opening of the container by a user, for example after lyophilization; thus facilitating recovery of the lyophilized product.

According to the invention, the product to be lyophilized is contained in body portion

102

. Neck

108

and stopper

110

serve to permit filling of the bulk lyophilization container and to permit vapor to escape at an appropriate step of the lyophilization process. After sufficient solvent has been removed from product

112

, stopper

110

may be pushed down into neck

108

, completely sealing the container.

FIG. 1B

further illustrates this arrangement. The product powder may be reconstituted with liquid through the neck

108

without opening the aseptic closure portion

104

.

FIG. 1C

is a cross-section of a bulk lyophilization container according to the invention, showing an alternative sealing arrangement. Shown are body portion

102

, aseptic closure portion

120

, seal

105

, product

112

, and sealable neck

122

. Aseptic closure portion

120

and seal

105

serve to form an aseptic barrier across the opening of body portion

102

. Sealable neck

122

permits product

112

to be filled aseptically into the bulk lyophilization container, and allows vapor to escape during lyophilization. After lyophilization, sealable neck

122

may be sealed by sealing equipment

124

, along the direction indicated by arrows

126

, to form an aseptic enclosure.

FIGS. 2A-F

show several exemplary embodiments of the inventive present invention, emphasizing seal configurations. In FIGS.

2

A-

2

D, the body portion

202

, aseptic closure portion

204

, neck

206

, stopper

208

, product

210

, stiffener

212

, seal

214

, C-clips

216

, and mechanical clamps

218

are indicated. Relative to the interior of the product receptacle,

FIG. 2A

shows a concave body portion

202

and convex aseptic closure portion

204

combination.

FIG. 2B

shows a concave body portion

202

and concave aseptic closure portion

204

configuration.

FIG. 2C

shows a flat body portion and concave aseptic closure portion

204

configuration, with spring clamps

218

.

FIG. 2D

shows a concave body portion

202

and flat aseptic closure portion

204

configuration, with stiffeners

212

to support neck

206

.

FIG. 2E

shows a concave body portion

202

and concave aseptic closure portion

204

configuration, with two necks

206

.

FIG. 2F

is an isometric view of the bulk lyophilization container embodiment shown in FIG.

2

E.

Multiple necks may permit faster removal of the water/solvent vapor (less flow resistance) during intensive lyophilization processes. This may be a consideration in the practice of the present invention in that the area through which vapor may flow during lyophilization may be reduced by the addition of the aseptic closure portion. Accordingly, multiple necks (or modified lyophilization stoppers, as discussed further below) may be utilized to increase the rate of bulk lyophilization when bulk lyophilization is being practiced according to the present invention. Multiple necks may also be built into trays with large surface areas.

FIGS. 3A-H

show several exemplary plan view geometries and array formations according to the present invention. In

FIGS. 3A-3D

, body portion

302

, covering element

304

, neck

306

, and stopper

308

are indicated.

FIG. 3A

shows a rectangular (quadrilateral) bulk lyophilization container according to the invention.

FIG. 3B

shows the rectangular (quadrilateral) bulk lyophilization container of

FIG. 3A

arranged in an array for compact storage.

FIG. 3C

shows a triangular bulk lyophilization container according to the invention.

FIG. 3D

shows the triangular bulk lyophilization container of

FIG. 3C

arranged in an array for compact storage.

FIG. 3E

shows a circular bulk lyophilization container according to the invention.

FIG. 3F

shows the circular bulk lyophilization container of

FIG. 3E

arranged in an array for compact storage.

FIG. 3G

shows an elliptical bulk lyophilization container according to the invention.

FIG. 3H

shows the elliptical bulk lyophilization container of

FIG. 3G

arranged in an array for compact storage. Various polygonal and non-polygonal geometries including, but not limited to, pentagonal, hexagonal, etc. beyond those shown will no doubt occur to one of skill in the art, and are within the scope of the invention.

FIGS. 4A-C

show exemplary alignment and supporting aids for vertical stacking of the bulk lyophilization containers according to the present invention.

FIGS. 4A-C

show body portion

402

, aseptic closure portion

404

, neck

406

, stopper

408

, edge support/alignment element

410

, support/alignment pin

412

, and raised center portion

420

. In

FIGS. 4A-B

, edge support/alignment element

410

or support/alignment pin

412

serve to align and support vertically stacked bulk lyophilization containers according to the invention. In

FIG. 4C

, raised center portion

420

serves to support vertically stacked bulk lyophilization containers according to the invention. Additional alignment or support configurations beyond those shown will no doubt occur to one of skill in the art, and are within the scope of the invention.

FIGS. 5A-5F

show exemplary locations of the neck according to the present invention. In

FIGS. 5A-C

, body portion

502

, aseptic closure portion

504

, seal

505

, neck

508

, stopper

510

, reinforcing stiffener

512

, and optional liquid ports

514

A-B are indicated.

FIG. 5A

shows an isometric view of an embodiment of the inventive bulk lyophilization container useful for lyophilization followed by reconstitution. Shown are body portion

502

integral with aseptic closure portion

504

, neck

508

, stopper

510

(located roughly centrally as shown, but potentially offset in certain embodiments with respect to the sides of the bulk lyophilization container, and shown in the open position, and reinforcing stiffeners

512

to reinforce and stiffen neck

508

.

FIG. 5B

shows the bulk lyophilization container of

FIG. 5A

in a cross-sectional view. Also depicted in

FIG. 5B

is product

516

, shown at a typical level within the embodiment of FIG.

5

B.

FIG. 5C

shows a cross-sectional view of an embodiment of the inventive bulk lyophilization container useful for lyophilization followed by reconstitution. Shown are body portion

502

integral with aseptic closure portion

504

, necks

508

, stoppers

510

, product

516

and reinforcement stiffener

520

. Two necks and stoppers are provided so that, for example, one neck may be used for introducing material and the other neck may be used as a vent. Two or more necks also increase the cross-sectional area through which vapor may be passed during lyophilization, thus decreasing lyophilization time. Such multi-neck embodiments may be useful in embodiments of the invention generally as is appropriate. Reinforcement stiffener

520

serves to reinforce neck

508

. Only one reinforcement stiffener may be present, or more than one may be present.

FIG. 5D

shows a cross-section of a bulk lyophilization container according to the invention, suitable for use in lyophilization and reconstitution. Shown are body portion

502

, aseptic closure portion

504

, seals

505

, neck

508

, stopper

510

, product

516

, and optional liquid ports

514

A-B. Seals

505

serve to couple body portion

502

and aseptic closure portion

504

. Neck

508

and stopper

510

are arranged and function as described above. Optional liquid ports

514

A-B are shown in a sealed configuration. Optional liquid ports

514

A-B may be used to empty reconstituted liquid from the bulk lyophilization container, for example by clipping the ends of the optional liquid ports to create an opening in the bulk lyophilization container. Alternatively, reconstituted liquid may be removed from the bulk lyophilization container by pouring it out of neck

508

or from liquid port(s)

514

A-B.

FIGS. 5E-F

show multi-neck embodiments if the inventive bulk lyophilization containers according to the invention. Two necks and stoppers are provided so that, for example, one neck may be used for introducing material and the other neck may be used as a vent. Two or more necks also increase the cross-sectional area through which vapor may be passed during lyophilization, thus decreasing lyophilization time. More than two necks are also contemplated as within the scope of the invention. Such multi-neck embodiments may be useful in embodiments of the invention generally as is appropriate. For example, more than the two shown necks may be utilized for large surface containers.

FIG. 5E

shows body portion

502

, aseptic closure portion

504

, seals

505

, neck

508

, stopper

510

, opening tab

518

, opening handle

520

, and scoring

522

. The structure and function of these elements are similar to those described above. In particular, opening tab

518

and opening handle

520

may be used to pull open body portion

502

along scoring

522

.

Stoppers

510

are shown as being in a closed position in

FIG. 5E

, and in an open position in FIG.

5

F. In the bulk lyophilization container embodiments according to the invention, the bulk lyophilization containers are preferentially of a height

524

(as shown in the exemplary embodiments of

FIGS. 5E-F

) that is suitable for use in conventional, preferably stoppering shelf-type lyophilizers. More preferably, the height

524

of the inventive bulk lyophilization containers is such that conventional stoppering shelf-type lyophilizers may be used to close stoppers

510

in necks

508

, thus sealing closed the inventive bulk lyophilization containers.

FIGS. 6A-B

show different views of a prior art lyophilization stopper. In

FIG. 6A

, which is a side view of a prior art lyophilization stopper, stopper body

602

and straight vent notch

604

are indicated. As is shown, the prior art lyophilization stopper possesses two straight vent notches

604

.

FIG. 6B

shows the prior art lyophilization stopper shown in

FIG. 6A

in an isometric view. Straight vent notches

604

permit the escape of vapor from a lyophilization container when the stopper is not pushed into and sealed against a neck of the lyophilization container.

FIG. 6C

shows a lyophilization stopper with three straight vent notches, including stopper body

606

, and straight vent notches

608

. The addition of a third straight vent notch provides a more open cross-sectional area through which vapors may pass during lyophilization. This additional cross-sectional area therefore serves to increase the flow rate of vapors out of the lyophilization container, and decrease the lyophilization time. While the innovation of increasing cross-sectional area for vapor passage is applicable to lyophilization stoppers generally, in a preferable embodiment such lyophilization stoppers are used with the inventive bulk lyophilization containers.

FIG. 6D

shows a cross-section taken as indicated by line A—A through the lyophilization stopper of FIG.

6

C. Shown are stopper body

606

, three straight vent notches

608

, and hollow center portion

610

, and arrangements of each relative to one another.

FIG. 6E

shows a lyophilization stopper with four straight vent notches, including stopper body

620

, and straight vent notches

622

. The addition of a fourth straight vent notch may increase the open cross-sectional area of the lyophilization stopper as compared to the lyophilization stoppers of

FIGS. 6A & 6C

. This additional cross-sectional area serves to further increase the flow rate of vapors out of the lyophilization container, and further decrease the lyophilization time.

FIG. 6F

shows a cross-section taken as indicated by line B—B through the lyophilization stopper of FIG.

6

E. Shown are stopper body

620

, four straight vent notches

622

, and hollow center portion

624

, and arrangements of each relative to one another.

FIG. 7A-L

show lyophilization stopper and vent embodiments according to the present invention. In

FIG. 7A-7G

, straight vent notch

712

, sealing ridges

720

, first stopper leg thickness

730

, second stopper leg thickness

740

, stopper leg end radius

750

, stopper leg

760

, stopper window vent

770

, stopper window vent reinforcing zones

772

, neck

774

, pierced neck

778

, neck window vents

780

, and unvented stopper

782

are illustrated.

FIG. 7A

shows a lyophilization stopper according to the present invention with stopper body

710

comprising sealing ridges

720

located on an outer surface along with straight vent notch

712

. Sealing ridges

720

provide a potentially better seal between the stopper and a neck of a lyophilization container when the stopper is pushed into the neck. Such a design is particularly useful for non-elastomeric lyophilization stopper materials. The sealing ridges may possess various cross sections, e.g. semi-circular, triangular, trapezoidal, square/rectangular, a split lip edge, etc. The individual width of these ridges may vary, e.g. they may have various cross section area and various elastic deformation to ensure collaborative performance among all ridges. The ridges may be separated or touch each other in the free or compressed state. The number of these ridges may vary depending on the stopper material, stopper diameter, length of storage, etc. The inventive lyophilization stoppers comprising sealing ridges may or may not additionally comprise straight vent notches.

FIG. 7B

shows another lyophilization stopper embodiment according to the present invention. Stopper legs

760

define straight vent notches

712

. Further, stopper legs

760

are stiffer than legs of the prior art stoppers as shown in

FIGS. 6A-6B

. The increased stiffness of stopper legs

760

may be accomplished by having a second stopper leg thickness

740

that is greater than a first stopper leg thickness

730

, as shown. Stopper leg end radii, such as stopper leg end radius

750

, may be utilized generally, as appropriate, in lyophilization stoppers according the invention to reduce folding of the stopper legs upon insertion into a neck of a lyophilization container.

FIG. 7C

shows a stopper according to the present invention including stopper window vents

770

. These vents may act as passages for the escape of vapor from bulk lyophilization containers and are arrayed about the circumference of the lyophilization stopper. The shape of the stopper window vents

770

may be as shown but is not limited to square/rectangle shape. The circular or oval stopper window vents may also be used. These vents may not only facilitate vapor passage during lyophilization, but also optimize the stopper behavior (deformation under stress and subsequent sealing) during the stoppering step. Various shapes and local reinforcing or weakening zones can further optimize stopper performance during drying, stoppering and storage (sealing).

FIG. 7D

shows another lyophilization stopper according to the invention. Shown are stopper window vents

770

, with window vent reinforcing zones

772

designed to reinforce the area around stopper window vents

770

. The window vent reinforcing zones

772

may be used to reduce distortions of stopper window vents

770

when the lyophilization stopper is under a load, such as when the stopper is being pushed into a neck of a lyophilization container.

FIG. 7E

shows an embodiment of the invention wherein a lyophilization stopper possessing stopper window vents is inserted into neck

774

. During lyophilization, vapor may pass through neck

774

and out of the stopper window vents

770

. At an appropriate time in the lyophilization process, the iyophilization stopper may be pushed into neck

774

forming a seal. A neck window vent embodiment is also within the scope of the invention.

FIG. 7F

shows pierced neck

778

comprising neck window vents

780

, with unvented stopper

782

. In this embodiment, vapor can flow through pierced neck

778

and out of neck window vents

780

. The neck window vents are sealed when unvented stopper

782

is pushed into pierced neck

778

far enough so as to seal off neck window vents

780

. The pierced neck may also facilitate the container filling with liquid windows in the neck permit liquid-displaced air/gas removal from the container.

FIG. 7G

shows a lyophilization stopper according to the invention. Cross-sections taken through line A—A result in the exemplary geometries shown in

FIGS. 7H-K

.

FIGS. 7H-I

show cross-sectional of lyophilization stoppers comprising shallow vents that do not pass completely though the lyophilization stopper. During lyophilization, vapor passes through a channel formed by the shallow vents and an interior surface of a neck within which the lyophilization stopper is present. The cross-section shown in

FIG. 7I

differs from that shown in

FIG. 7H

in that the cross-section shown in

FIG. 71

possesses a hollow central area, whereas the cross-section shown in

FIG. 7H

possesses a solid central area.

FIGS. 7J-K

also show cross-sections of lyophilization stoppers comprising shallow vents that do not pass completely though the lyophilization stopper. The shallow vents shown in

FIGS. 7J-K

differ from the vents shown in

FIGS. 7H-I

in shape, and the cross-sectional area of the vents may be different or the same. Shallow vents as shown in these embodiments offer an equivalent structure to the vents shown in the embodiments of

FIGS. 6C-F

and

7

A-F.

FIG. 7L

shows spiral vents to facilitate stopper insertion during stoppering. Other arrangements will no doubt occur to one of skill in the art and are expressly within the scope of the invention.

FIGS. 8A-8E

show exemplary edge sealing embodiments of bulk lyophilization containers according to the present invention. In

FIGS. 8A-D

, compressing member

810

, aseptic covering portion

812

, body portion

814

, product

816

, lyophilization stopper

818

, edge sealing element

820

, neck

822

, rotating catch

824

, flat gasket

830

, clamp

832

, first sealing surface

840

, second sealing surface

842

, third sealing surface

844

, circular gasket

846

, fourth sealing surface

855

, and cover alignment aids

860

are indicated.

In

FIG. 8A

, compressing member

810

is shown bearing upon lyophilization stopper

818

to seal it against neck

822

. As well, compressing member

810

bears upon aseptic covering portion

812

and compresses edge sealing element

820

to form a seal along the edge of body portion

814

. Rotating catch

824

serves to hold aseptic covering portion

812

against body portion

814

, thus keeping edge sealing element

820

under compression and maintaining the seal. Contamination of product

816

is thus reduced.

FIG. 8B

illustrates the compression of edge sealing element

820

by the contacting surfaces of aseptic covering portion

812

and body portion

814

.

FIGS. 8C-E

show alternate embodiments of edge seals for bulk lyophilization containers according to the present invention. In

FIG. 8C

, the edge seal is formed by the compression of flat gasket

830

by aseptic covering portion

812

and body portion

814

. The seal is maintained by the action of clamp

832

.

FIG. 8D

is an edge sealing embodiment of an inventive bulk lyophilization container with more than two sealing surfaces.

FIG. 8E

shows first and second sealing surfaces

840

and

842

, and a third sealing surface

844

. Under compression, circular gasket

846

forms an additional seal with third sealing surface

844

.

FIG. 8D

shows another embodiment of edge seals according to the present invention. In this embodiment, circular gasket

846

is contained in a groove. Upon compression, circular gasket

846

will form seals against four surfaces

850

,

852

,

854

and

856

.

FIG. 8F

illustrates cover alignment aids

860

. Alignment aids

860

assist in positioning of the circular gasket

846

over body portion

814

in order to properly form edge seals.

FIGS. 9A-E

show exemplary embodiments of edge seal-vents for bulk lyophilization containers according to the present invention.

FIG. 9A

shows edge vents

902

, tabs

904

, and edge sealing element

906

. Edge vents

902

are coupled to edge sealing element

906

and provide a path for vapor to travel through during lyophilization. Tabs

904

are also coupled to edge sealing element

906

and define edge vents

902

. Tabs

904

may be coupled to a body portion either slidably or nonslidably. Under compression, edge vents

902

are squeezed closed, and edge sealing element

906

forms a seal.

This is better illustrated in FIG.

9

B. Shown are edge vents

902

, edge sealing element

906

, aseptic closure portion

908

, body portion

910

, and vapor path

912

. As shown in

FIG. 9B

, when uncompressed, edge vents

902

allow vapor to escape along vapor path

912

. This vapor path may be in addition to a vapor path through a neck or stopper, or it may be the sole vapor path. Upon compression, edge vents

902

are closed and a seal is formed between aseptic closure portion

908

and body portion

910

by edge sealing element

906

. This blocks vapor path

912

. Vent collapse generally does not occur without a compression force “F”.

FIGS. 9C-E

show how vapor path

912

is closed off as aseptic closure portion

908

and body portion

910

are brought together.

FIGS. 9F-H

show cross sections of different embodiments of edge sealing gaskets according to the invention. Shown are aseptic closure portion

908

, body portion

910

, bi-lobe sealing elements

920

, first tab

922

, second tab

924

, and third tab

926

. The bi-lobes of the bi-lobe sealing elements

920

may be arranged such that they straddle a tab designed to permit vapor flow through vapor path

912

to pass through the tab. The tab arrangement may vary according to various design considerations. For example, first tab

922

may extend towards an outside surface of the bulk lyophilization container. Alternatively, second tab

924

may extend towards an inside surface of the bulk lyophilization container. Finally, third tab

926

may be designed such that it may collapse between the bi-lobes of bi-lobe sealing elements

920

. In each of these embodiments, when bi-lobes of bi-lobe sealing elements

920

are under compression between aseptic closure portion

908

and body portion

910

, they serve to form a seal, both inner and outer, against possible contamination or leakage.

FIGS. 9I-M

show cross-sections of different embodiments of edge sealing gaskets according to the invention. Shown are edge sealing elements

930

, vapor vent

932

, and tab

934

.

FIG. 9G

shows these elements in relation to one another in an embodiment of the invention.

FIGS. 9H-I

show these elements in relation to aseptic closure portion

908

and body portion

910

. When aseptic closure portion

908

and body portion

910

do not compress the edge sealing gasket according to the invention, vapor may exit along vapor path

912

during lyophilization. Following lyophilization, aseptic closure portion

908

and body portion

910

may be moved together as indicated in

FIG. 9I

, compressing edge sealing elements

930

and interrupting vapor path

912

.

FIGS. 9J-K

show an alternative embodiment, wherein aseptic closure portion fasteners are used to maintain compression of edge sealing elements

930

. Movable member

944

may be moved downward to first notch

942

, which it then engages. Once engaged, movable member

944

holds aseptic closure portion

908

and second notch

940

holds body portion

910

such that edge sealing elements

930

are under compression. This cuts off vapor path

912

, as is shown by comparison between

FIGS. 9J and 9K

.

FIG. 10

shows an exemplary embodiment of aseptic closure portion fasteners for use with bulk lyophilization containers according to the present invention.

FIGS. 10A-10C

show aseptic closure portion

1010

, body portion

1020

, product

1022

, fastener

1030

, edge sealing element

1040

and vapor path

1050

. Fastener

1030

functions by holding together aseptic closure portion

1010

and body portion

1020

so as to keep edge sealing element under compression. When fastener

1030

does not hold together aseptic closure portion

1010

and body portion

1020

, vapor may travel along vapor path

1050

, thus facilitating lyophilization. When fastener

1030

holds together aseptic closure portion

1010

and body portion

1020

, vapor travel along vapor path

1050

is blocked.

FIG. 11A

illustrates the problem of heat flux management in a bulk lyophilization system. In

FIG. 11A

, shelf

1110

, body portion

1120

, product

1130

, heat conductor element

1136

, heat flux vectors

1150

A-C and contact points

1160

A-C are illustrated. In the process of bulk lyophilization, it is necessary that be removed from and added to product

1130

. These heat fluxes are effectuated primarily through conductive heat transfer between product

1130

and shelf

1110

via heat conductor element

1136

, of which body portion

1120

is comprised. In the course of repeated use, body portion

1120

and shelf

1110

do not remain planar and have a irregular mating surface with respect to one another. Typically, body portion

1120

will contact the shelf at a finite number of contact points, such as depicted by contact points

1160

A-C. Variations in the heat flux vectors

1150

(either from the body portion to the shelf or from the shelf to the body portion) occur across the base of the product receptacle because the mating between the shelf and the body portion is irregular.

To improve product quality and product uniformity, it is desirable to make uniform the heat flux from and to the product. The uniformity of heat transfer between the cooled/heated shelf of the lyophilizer and the product is of significance during freezing prior to lyophilization and during primary and secondary drying. During initial cooling and freezing, the uniform heat flux between the container wall facing the product and the product itself may determine the pattern of growing ice crystals, e.g. the pattern of ice crystals inside the frozen product matrix. Such a uniform heat flux may prevent local overcooling and localized initiation of ice crystal growth. The frozen matrix of ice crystals and product/solutes glassy states and eutectics between the ice crystals may determine the ice sublimation uniformity and the product/solutes matrix after the sublimation of ice step. In short, uniform heat flux during freezing may deliver uniform ice crystal matrix and uniform distribution of product and solutes between the ice crystals.

Uniform ice crystal structure tends to lead to uniform sublimation (sublimation ends at the same time for all areas of the container) and the resulting structure of the product and solutes solid therefore also may be uniform. Such uniform structure may permit uniform removal of the water/solvent from that matrix during secondary drying. Uniform heat flux may be helpful during secondary drying to reduce local overheating of the matrix (local overheating of the matrix may cause product softening in those areas, potentially leading to localized matrix collapse). Therefore, very uniform heat flux may be beneficial to the process during cooling, freezing, and primary and secondary drying.

As the contact between the cooling/heating shelf may not be uniform, thermal conductor element

1136

in the container bottom redistributes the heat flux and makes it more uniform on the product contact side.

FIG. 11B

shows one way of making the heat flux between a shelf and the product more uniform. Shown are shelf

1170

, containing bulk lyophilization containers

1172

, and liquid heat transfer media

1174

. Liquid heat transfer media

1174

conforms to the surface of both shelf

1170

and bulk lyophilization containers

1172

, thus making more uniform the heat transfer. However, this arrangement may create cleaning and contamination problems, due to the presence of liquid heat transfer media

1174

on the outside of bulk lyophilization containers

1172

and associated droplets and spills.

FIGS. 12A-F

show exemplary embodiments of heat flux management for bulk lyophilization containers according to the present invention.

FIG. 12A

shows shelf

1210

, body portion

1212

, product

1214

, aseptic closure portion

1216

, and heat flux equalizer portion

1218

. Enclosed by body portion

1212

and aseptic closure portion

1216

is product

1214

. Located on a bottom surface of body portion

1212

is heat flux equalizer portion

1218

. Heat flux equalizer portion

1218

improves the uniformity of the heat flux to the product

1214

from the shelf

1210

by virtue of relatively rapid isotropic heat conduction within heat flux equalizer portion

1218

. Heat flux equalizer portion

1218

is desirably located between product

1214

and shelf

1210

. Heat flux equalizing portions according to the invention may comprise a variety of materials, including phase change materials, and thermally conductive solid materials. Examples of thermally conductive solid materials include, but are not limited to, thermally conductive metals such as copper, aluminum, stainless steel, corrosion-resistant alloys, and titanium etc, and thermally conductive polymers. The thickness and attachment of such materials may be varied to improve the heat flux equalization imparted. The heat flux equalizer according to the invention may equalize heat flux in three dimensions, serving to provide both vertical and horizontal equalizing with respect to a shelf or tray of a tray lyophilizer. Further, the heat flux equalizing portion may possess linear or nonlinear heat flux or temperature change characteristics. Nonlinearities may be represented as a single curve in a plot of product temperature or heat flux to the product versus time or input heat flux. Nonlinearities may be represented as multiple curves, and therefore may exhibit hysteresis.

FIG. 12B

shows an alternate embodiment of the heat flux management according to the present invention including shelf

1210

, body portion

1220

, product

1214

, heat flux equalizer portion

1218

, aseptic closure portion

1222

, clamp

1224

, and seal

1226

. Clamp

1224

and seal

1226

serve to keep body portion

1212

and aseptic closure portion

1222

together so as to contain product

1214

. Heat flux equalizer portion

1218

improves the uniformity of the heat flux to the product

1214

from the shelf

1210

by virtue of relatively rapid isotropic heat conduction within heat flux equalizer portion

1218

.

FIG. 12C

shows an alternate embodiment of the heat flux management according to the present invention including shelf

1210

, body portion

1230

, phase change material

1234

, phase change material container

1232

, product

1214

, and aseptic closure portion

1236

. Enclosed by body portion

1230

and aseptic closure portion

1236

is product

1214

. Located on a bottom surface of body portion

1230

is phase change material

1234

, which may be enclosed or encapsulated by phase change material container

1232

. Phase change material

1234

represents a particular embodiment of a heat flux equalizer portion.

Phase change material

1234

may be such that it creates plateaus in the variation of heat flux from shelf

1210

to product

1214

versus time. The plateaus occur at a temperature range characteristic of the phase change material. There are a variety of phase change materials that may be enclosed by the phase change material container. In a preferable embodiment, the phase change material may have a transition temperature slightly below zero deg C. to reduce liquid undercooling during initial freezing, by slowing down the temperature decrease (e.g. providing a temperature plateau to equilibrate the product solution).

The phase change temperature may be also selected near the eutectic and glass transition temperatures where heat capacity of the matrix changes to absorb those changes and reduce sudden product temperature changes in those zones. This may make the transition smooth without product overheating, thus reducing the likelihood of resulting matrix softening and collapse, e.g., product thermal protection. The phase change material may absorb/supply additional heat flux over a narrow temperature range, for example, by melting, solidification or sublimation and vice versa. The phase change material thus may provide a way of thermal management and protection of product matrix in the transitional zones (with changing properties of product and solutes) where steady heat flux may cause sudden temperature changes.

The enclosed phase change material may include aqueous solutions (salts, molecular species), paraffins, gels, organic fluids, emulsions, etc. Preferably, such materials are encapsulated and sealed, thus reducing the possibility of leakage into the product. Expansion and contraction of these materials may be accommodated by providing side pockets on the tray circumference reaching beyond the product contact perimeter (e.g. without affecting the passage for the heat flux shelf-tray structure-product).

FIG. 12D

shows an alternate embodiment of the heat flux management according to the present invention including shelf

1210

, body portion

1248

, product

1214

, phase change material

1234

, phase change material container

1240

, aseptic closure portion

1242

, clamp

1244

, and seal

1246

. Clamp

1244

and seal

1246

serve to keep body portion

1248

and aseptic closure portion

1242

together so as to contain product

1214

. Located on a bottom surface of body portion

1248

is phase change material

1234

, which is enclosed by phase change material container

1240

. Phase change material

1234

is such that it creates plateaus in the variation of heat flux from shelf

1210

to product

1214

versus time, as discussed above.

FIGS. 12E-F

show different arrangements of heat flux equalizer portions on bulk lyophilization containers according to the invention. In

FIG. 12E

, heat flux equalizer portion

1250

is coupled to the bottom of body portion

1252

and is located between body portion

1252

and shelf

1210

. In

FIG. 12F

, heat flux equalizer portion

1260

is coupled to the bottom of body portion

1262

and is also coupled to the side

1264

and lip

1266

of body portion

1262

. This facilitates even heating along the bottom, and sides of product contained within the bulk lyophilization container. It may also facilitate tray manufacturing.

FIGS. 13A-C

show cross-sections of bulk lyophilization containers according to the invention. In

FIG. 13A

are shown body portion

1304

, neck

1308

, stopper

1310

, product

1316

, phase change material

1318

, phase change material container

1302

, aseptic closure portion

1306

, clamps

1314

, and seals

1312

. Clamps

1314

and seals

1312

serve to keep body portion

1304

and aseptic closure portion

1306

together so as to contain product

1316

. Stopper

1310

is located in neck

1308

, and permits vapor to flow through during lyophilization and may seal the neck following lyophilization. Located on a bottom surface of body portion

1304

is phase change material

1318

, which is enclosed by phase change material container

1302

. Phase change material

1318

is such that it creates plateaus in the variation of heat flux across its thickness to product

1316

versus time. The plateaus occur at a temperature range characteristic of the phase change material, as discussed above.

FIG. 13B

shows a cross section of an alternative embodiment of a bulk lyophilization container according to the invention. Shown are body portion

1326

, product

1316

, phase change material

1318

, phase change material container

1322

, aseptic closure portion

1320

, and sealing portions

1324

. Sealing portions

1324

serve to keep body portion

1326

and aseptic closure portion

1320

together so as to contain product

1316

. In this embodiment, sealing portions

1324

are designed such that they are semi-permanent in nature, and are less easily removed than clamp-based seals, for example. Located on a bottom surface of body portion

1326

is phase change material

1318

, which is enclosed by phase change material container

1322

. Phase change material

1318

is such that it creates plateaus in the variation of heat flux across its thickness to product

1316

versus time. The plateaus occur at a temperature range characteristic of the phase change material, as discussed above.

FIG. 13C

is an expanded cross-sectional view of the bulk lyophilization container of FIG.

13

A. The components, their structure and function are identical to the bulk lyophilization container of

FIG. 13A

, with the exception that lyophilized product

1330

is shown on body portion

1304

. Lyophilized product

1330

may be removed from body portion

1304

by sweeping or scraping it, for example, in the direction indicated by arrow

1332

as the surface may be substantially flat.

FIGS. 14A-H

show cross-sectional views of different sealing arrangements for bulk lyophilization containers according to the invention. Each seal serves to keep together the body portion and the aseptic closure portion.

FIG. 14A

shows seals formed by clamps

1402

and o-rings

1404

.

FIG. 14B

shows seals formed by removable foil

1406

.

FIG. 14C

shows seals

1408

formed by thermoforming processes, such as those involving rolling and compressing. Such seals

1408

may be formed by heat sealing of polymers or heat sealing of multilayer materials, for example a foil or metal sheet covered with a thermosealing layer. Seals

1408

may also be made using pressure-sensitive sealants, or heat and compression techniques.

FIG. 14D

shows single-use seals

1410

. Various types of these single-use seals are shown in enlarged detail in

FIGS. 14E-H

. Shown in

FIG. 14E

is tack-welded seal

1412

. Shown in

FIG. 14F

is notched wall seal

1414

. Shown in

FIG. 14G

is notched corner seal

1416

. Shown in

FIG. 1418

is notched bottom seal

1418

. A notched design may provide improved bottom removal for product emptying from single-use trays.

FIGS. 15A-E

show cross-sections of lyophilization vials using heat flux equalizer portion according to the invention. These embodiments show that the heat flux equalizer portions may be applied to conventional lyophilization vials or containers with improved lyophilization results.

FIG. 15A

shows a cross-section of conventional lyophilization vial or container

1502

coupled to heat flux equalizer portion

1504

. Heat flux equalizer portion

1504

possesses a thickness sufficient to improve the uniformity of the heat flux across its thickness.

FIG. 15B

shows an expanded view of a portion of the embodiment shown in FIG.

15

A.

FIG. 15C

shows a cross-sectional view of another embodiment, showing a different arrangement of conventional lyophilization vial or container

1506

coupled to heat flux equalizer portion

1508

.

FIG. 15D

shows a cross-sectional view of another embodiment, showing a different arrangement of conventional lyophilization vial or container

1506

coupled to heat flux equalizer portion

1510

.

FIG. 15E

shows a cross-sectional view of another embodiment, showing a different arrangement of conventional lyophilization vial or container

1506

coupled to heat flux equalizer portion

1512

. These reduced or expanded areas of thermal conductor may depend on the type of the container wall used to compensate for differences in thermal conductivity between the product and the material of container wall. Good contact between the container/vial bottom material and high thermal conductivity layer is preferable, e.g. there preferably are few to no gaps/crevices there. In a more preferable embodiment, the container wall and the high thermal conductivity layer of the heat flux equalizer portion may be fused. The vial production process may be mass-automated to include permanent attachment of the bottom equalizer.

It will be apparent to those skilled in the art that various modifications and variations can be made in the lyophilization apparatus and methods of the present invention without departing from the spirit or scope of the invention. Thus, it is intended that the present invention cover the modifications and variations of this invention provided they come within the scope of the appended claims and their equivalents.

Claims

1. A bulk lyophilization container comprising:a body portion; and an aseptic closure portion, wherein the body portion is coupled to the aseptic closure portion; and the aseptic closure portion comprising an impervious membrane detachably coupled to the body portion via a membrane seal, wherein the impervious membrane may be detached from the body portion by tearing the membrane.
2. A bulk lyophilization container comprising; a body portion;an aseptic closure portion; and at least two filling/ventilating necks; wherein the body portion is detachably coupled to the aseptic closure portion, thereby facilitating removal of lyophilized product after lyophilization.
3. The bulk lyophilization container of claim 2, wherein the aseptic closure portion is detachably coupled to the body portion by at least one mechanical clamp.
4. A bulk lyophilization container comprising:a body portion; and an aseptic closure portion, wherein the body portion is coupled to the aseptic closure portion and the aseptic closure portion comprises a sealable neck, and the sealable neck capable of being sealed after lyophilization of a product contained in the bulk lyophilization container.
5. A bulk lyophilization container comprising:a body portion; and an aseptic closure portion, wherein the body portion is non-detachably coupled to the aseptic closure portion and wherein the bulk lyophilization container is stiff thereby improving lyophilization of a product contained in the bulk lyophilization container.
6. A bulk lyophilization container comprising:a body portion; an aseptic closure portion; and at least one filling/ventilating neck, wherein the at least one filling/ventilating neck is mechanically reinforced to facilitate filling of a product or ventilation of vapors during lyophilization; and wherein the body portion is coupled to the aseptic closure portion.
7. A bulk lyophilization container comprising:a body portion; an aseptic closure portion; and at least one filling/ventilating neck; and wherein the body portion is coupled to the aseptic closure portion, and the container is stiff thereby improving lyophilization of a product contained in the bulk lyophilization container.
8. A bulk lyophilization container comprising:a body portion; and an aseptic closure portion, wherein the body portion is coupled to the aseptic closure portion, and the bulk lyophilization container being stiff thereby improving lyophilization of a product contained in the bulk lyophilization container and the bulk lyophilization container possessing a geometric shape suitable for compact storage.
9. The bulk lyophilization container of claim 8, wherein the geometic shape includes a circular, triangular, elliptical, quadrilaterial, pentagonal, or hexagonal shape.
10. An array comprising bulk lyophilization containers, wherein the bulk lyophilization containers comprise:a body portion; and an aseptic closure portion; wherein the body portion is coupled to the aseptic closure portion, and the bulk lyophilization container being stiff thereby improving lyophilization of a product contained in the bulk lyophilization container and the bulk lyophilization container possessing a geometric shape suitable for compact storage.
11. A method of storing lyophilized material, comprising:storing the lyophilized material in bulk lyophilization containers; wherein the bulk lyophilization containers comprise a body portion; and an aseptic closure portion; wherein the body portion is coupled to the aseptic closure portion, and the bulk lyophilization container being stiff thereby improving lyophilization of a product contained in the bulk lyophilization container and the bulk lyophilization container possessing a geometric shape suitable for compact storage.
12. A bulk lyophilization container comprising:a body portion; an aseptic closure portion; and alignment or supporting aids coupled to the bulk lyophilization container; wherein the body portion is coupled to the aseptic closure portion and the bulk lyophilization container being stiff thereby improving lyophilization of a product contained in the bulk lyophilization container.
13. The bulk lyophilization container of claim 12, wherein the alignment and support aids comprise edge support/alignment elements, support/alignment pins or raised center portions.
14. A bulk lyophilization container comprising:a body portion; an aseptic closure portion; and optional liquid ports coupled to the bulk lyophilization container to facilitate addition or removal of liquid after lyophilization; wherein the body portion is coupled to the aseptic closure portion.
15. A bulk lyophilization container comprising:a body portion; and an aseptic closure portion, wherein the body portion is coupled to the aseptic closure portion via seals comprising seals formed by clamps and o-rings thereby facilitating removal of lyophilized product from the bulk lyophilization container following lyophilizaton.
16. A bulk lyophilization container comprising:a body portion; and an aseptic closure portion; wherein the body portion is coupled to the aseptic closure portion via seals comprising seals formed by removable foil, thermoforming, heat sealing of polymers or heat sealing of multilayer materials, pressure-sensitive sealants, heat and compression techniques, or single-use seals.
17. The bulk lyophilization container of claim 16, wherein the single-use seals comprise a tack-welded seal, a notched wall seal, a notched corner seal, or a notched bottom seal.
18. A bulk lyophilization container comprising:a body portion; an aseptic closure portion; and an edge sealing element coupled to tabs; wherein the tabs and the edge sealing element define edge vents such that the edge vents provide a path for vapor to travel through during lyophilization, and wherein the aseptic closure portion and the body portion are coupled via the edge sealing element coupled to the tabs, and wherein the edge sealing element serves to form a seal between the aseptic closure portion and the body portion when the aseptic closure portion and the body portion are compressed together.
19. A bulk lyophilization container comprising:a body portion; an aseptic closure portion; and a bi-lobe sealing element coupled to tabs; wherein the tabs are designed to permit vapor flow to pass through or around the tabs during lyophilization, and wherein the aseptic closure portion and the body portion are coupled via the bi-lobe sealing element coupled to the tabs, and wherein the bi-lobe sealing element serves to form a seal between the aseptic closure portion and the body portion when the aseptic closure portion and the body portion are compressed together.
20. The bulk lyophilization container of claim 19, wherein the tabs extend towards an outer surface of the bulk lyophilization container.
21. The bulk lyophilization container of claim 20, wherein the tabs extend towards an inner surface of the bulk lyophilization container.
22. The bulk lyophilization container of claim 21, wherein the tabs are arranged such that they collapse between bi-lobes of the bi-lobe sealing elements.
23. A bulk lyophilization container comprising:a flat body portion wherein the flat body portion facilitates removal of lyophilized product from the bulk lyophilization container following lyophilization; and an aseptic closure portion; wherein the body portion is coupled to the aseptic closure portion.
24. A bulk lyophilization container comprising:a body portion; and a flat aseptic closure portion wherein the flat aseptic closure portion facilitates removal of lyophilized product from the bulk lyophilization container following lyophilization; wherein the body portion is coupled to the aseptic closure portion.

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Non-Patent Literature Citations (1)

Entry
Hashimoto, S.; “Patent Abstract of Japan”; vol. 5, No. 35; JP 55 159776; Mar. 5, 1981, abstract.

Lyophilization apparatus and methods

Information

Patent Number

Date Filed

Date Issued

Inventors

Original Assignees

Examiners

Agents

CPC

US Classifications

Field of Search

US

International Classifications

Abstract

Description

Claims

US Referenced Citations (11)

Foreign Referenced Citations (4)

Non-Patent Literature Citations (1)