DE102010050242A1 - Drug package for delivery of drugs, and for encapsulation and storage of fragrances and chemical indicators, comprises impermeable surface shaped cavity made of thin glass, where cavity is provided for containing active ingredient - Google Patents

Abstract

The drug package comprises an impermeable surface shaped cavity (2) made of thin glass, where the cavity is provided for containing an active ingredient. The cavity has a specific wall thickness, and is formed from a largely alkali-free thin glass or a stained thin glass, particularly a brown glass. The inner wall of the cavity is coated with a barrier layer, particularly a silicon dioxide layer.

Description

Field of the invention

The present invention relates to a drug package in the form of a sheet-like cavity of thin glass in which an active ingredient is contained and which is breakable for dispensing the active ingredient. The cavity is enclosed in particular in a transdermal patch or in a shell, which can deliver the active ingredient in a controlled manner.

Background of the invention

Drug patches are known as transdermal patches or as a transdermal therapeutic system (TTS) for the delivery of drugs in patch form. As a transdermal patch it is stuck to the skin, so that the active ingredients get controlled directly through the skin into the blood vessel system, without being prematurely degraded in the gastrointestinal tract or in the liver.

Transdermal patches have been used for many years for various purposes. Examples are drug patches in pain therapy, nicotine patch for smoking cessation, scopolamine patches against motion sickness, clonidine patch for hypertension or hormone patch, which is a hormone administration z. B. in hormone replacement therapy.

The structure of such patches is different because of the different active ingredients. Here are two types of plasters differ. On the one hand, a matrix plaster as in the example DE 33 15 272 is described. The active ingredient is contained as a solution in a polymer matrix consisting of several layers, which can be applied directly to the skin with the aid of a contact adhesive layer permeable to the active substance. The pressure-sensitive adhesive layer is covered with a removable protective film, which is removed before the application of the active substance plaster. On the side opposite the pressure-sensitive adhesive layer of the plaster, a cover layer impermeable to the active substance is arranged.

Another type of patches is a membrane patch such as the DE-OS 2,135,533 describes. The drug reservoir may be formed as a hollow drug container or form a solid matrix or gel matrix in which the drug is evenly distributed. The drug is delivered through the reservoir wall to an adhesive layer, the release rate being controlled by the composition and thickness of the reservoir wall, which is configured as a solubility membrane. The drug reservoir may be disposed as a layer over the adhesive layer or as a microcapsule dispersed in the adhesive layer.

A disadvantage of both systems is that the active ingredient is exposed in all cases to the entry of environmental influences. In particular, these are components of the ambient air such as moisture or oxygen, but also impurities that can diffuse through the air or moisture in such a patch, can react with the active ingredient or contaminate it.

The pharmaceutical industry is working intensively on administering drugs transdermally via so-called active substance patches. However, the developers of the active ingredient patch are still facing the problem that decay-critical agents that react, for example, with components of the air such as moisture or oxygen, can not be protected in glass vials or pre-filled glass syringes from environmental influences, as is possible for injectable drugs.

Also, the contact of many drugs with the polymer materials proposed in the prior art is not desirable, since it comes to a reaction or to an undesirable diffusion of substances from a drug-defining plastic in the drug.

In order to avoid damage to a light-sensitive active substance contained in a transdermal patch by exposure to light, it is already known to cover the side of the active ingredient-containing matrix remote from the skin, exposed to the light, with a suitable protective material. That's how it describes DE 199 12 623 a method for increasing the stability during storage and / or application of photosensitive therapeutic systems or their constituents, such as active ingredients or auxiliaries, using light-shielding substances which absorb or reflect electromagnetic waves. Thus, a cover is described by a brown-colored film whose Absorbtionspektrum includes the wavelength, which is responsible for the drug degradation. Furthermore, in such films z. B. opalescent substances such as titanium oxide may be incorporated or the films may be aluminized.

Furthermore, the describes DE 199 12 623 a dosage form in which the stability of photosensitive members or components is significantly enhanced by means for preventing the ingress of stability-affecting components such as air, water and / or light by comprising materials such as glass, films, polymers, etc., the absorption or release of which Reflection spectrum includes the wavelength range, which is responsible for the degradation of active ingredients or excipients, and at least are impermeable to the ingress of air and light. However, DE 199 12 623 in any way an indication, such. B. such glass means should be designed, used or arranged.

Other embodiments for increasing the storage stability by protection against the effects of light, air and moisture are known and described in the literature.

That's how it describes WO 91/09 731 a packaging material that should be suitable for long-term storage of nicotine preparations. To produce the packaging material, a laminate is used which serves as a barrier and at least reduces the diffusion of oxygen and moisture and the action of light. However, the proposed solution is limited to the use of special transdermal patches for nicotine and not universally applicable.

The DE 36 50 575 describes a transdermal patch for the administration of nicotine. This consists of a carrier film, a nicotine-permeable membrane or a nicotine-permeable film, a nicotine-containing matrix or gelatinous base and an adhesive for fixing the patch on the. Skin. It is characteristic that the carrier or sealing film is impermeable to air, water and light. The light and air impermeability protects the nicotine from degradation and the water impermeability prevents nicotine diffusion. It is suggested to seal the patch in an airtight bag prior to use to prevent the reaction between nicotine and air.

The US 5,008,110 describes a transdermal patch, for example for the application of buprenorphine. It is characteristic that the transdermal therapeutic system (TTS) drug contained in the storage state prior to use is enclosed in a hermetically sealed chamber which protects the formulation from environmental factors such as moisture, oxygen and light. This chamber is formed of upper and lower cover sheets, which are heat-sealed together for sealing. The films consist of a laminate of an outer heat sealable polyolefin layer, an environmental barrier such as polyester, metal (aluminum) foil, metallized polyester or PVC, and an inner heat-sealable polyolefin layer. This measure increases the stability of the preparation and the efficiency. For use of the patch, the upper cover sheet is peeled off, thereby opening the chamber to release the active ingredient.

Another disadvantage of this solution is that it can only be used for specific active ingredients. Many other agents react with the materials of the cover sheets of the chamber or substances from the cover materials diffuse into the active ingredient. Also, the cover sheets themselves are not really diffusion-tight, neither for possible components of an active ingredient nor for components of the ambient air.

A long-term and safe protection against the adverse effects on drugs in general by light, oxygen and moisture is not guaranteed.

The described measures provide more general protection. It uses films or laminates that are components of the primary packaging or the therapeutic system. It is characteristic that these measures do not offer specific protection, but rather aim to protect the therapeutic systems in general from environmental influences. In this context, the factors air, water and light are called.

The causes that cause the instability of a drug form are twofold. On the one hand, it is the instability of the pharmaceutical and excipients themselves that ultimately results from their chemical or physicochemical structure; on the other, it is the external factors such as temperature, humidity, atmospheric oxygen and light that induce or accelerate reactions that reduce the effects of chemicals. The extent to which these factors are effective depends to a large extent on the composition of the active substance. In general, a distinction can be made between physical, chemical and biological instability.

Physical stability-impairing processes can be, for example, changes in the crystal structure, change in the distribution state, change in the consistency or state of aggregation, change in the solubility ratios or change in the hydration ratios.

Durability-impairing chemical reactions are, for example, hydrolysis, oxidation, reduction, steric rearrangements or else decarboxylations or polymerizations.

In practice, an exact allocation of instability to one of these categories is often not possible because it is often a complex interaction, the results of which only become detectable or perceptible through the end effect.

In known stabilization measures the sunscreen is essential. Light exposure can increase the stability of an active Active substance itself, but also affect the stability of adjuvants used. Investigations have shown that for instabilities caused by light, only a certain spectral range of the light is responsible. It was also shown that the most effective light protection is achieved by substances or measures whose absorption maxima are in the range of those wavelengths which are mainly responsible for the degradation. For example, the storage of oxidation-sensitive substances in opaque or partially translucent containers, such. As in porcelain jars or containers made of brown glass, well known and absolutely necessary to ensure adequate storage stability.

However, z. As ampoules or vials no solution for areal applications and can not be integrated into an active ingredient patch.

Object of the invention

The object of the invention is thus to overcome the disadvantages and to provide a sheet-like active ingredient packaging that is versatile and can be used for a wide range of drugs that provides reliable protection of the drug from environmental influences, for the drug is diffusion-tight and is suitable for this application easy to integrate into an active ingredient patch.

Description of the invention

According to the invention, the object indicated above is achieved by the characterizing features of the first claim and specified by the characteristics of the dependent claims 2 to 15. An active ingredient package produced by the process according to the invention results from the characterizing features of claims 16 to 20.

According to the invention, a drug package in the form of a sheet-like cavity, a sheet-like cavity made of thin glass is provided, in which an active ingredient can be stored protected. To deliver the drug, the cavity can be broken.

First of all, all the advantages of glass come into their own, as far as the barrier effect against diffusion of air components such as oxygen or moisture is concerned, but also against diffusion of constituents of the active substance outwards. On the other hand, glass is in a known manner inert to reactions of constituents of the active ingredient or the active ingredient itself, so that a long shelf life of the active ingredient is ensured in the packaging, which is limited only by the instability of an active ingredient itself or of components thereof.

To increase the shelf life even further, the thin glass panes on the active ingredient contact side can be coated with an additional barrier layer. This may consist of pure SiO ₂ , as it is also the prior art in the packaging of pharmaceuticals in ampoules and vials. In particular, such a coating prevents the diffusion of ions such. As alkalis from the glass in the drug.

In another embodiment, the thin glass panes on the side facing away from the active substance are coated with a UV-reflecting layer in order to protect the active ingredient against damaging UV radiation, ie. H. Protect against harmful electromagnetic waves in the spectral range less than 380 nm and against short-wavelength radiation in the spectral range of less than 420 nm in the visible wavelength range.

Such UV protective layers of at least four individual layers, in particular of five individual layers, are for example in EP 1 248 959 B1 "UV-reflecting interference layer system" described in the disclosure of which reference is made in its entirety and the disclosure of which is part of this application. But also all other coating systems known to those skilled in the art are applicable.

In particular, an additional UV protection with such a barrier layer is advantageous. As is known, many active substances suffer in some cases considerable damage due to the action of radiation, especially in the harmful UV-B range from 315 nm to 280 nm and also in the UV-A range from 380 to 315 nm EP 1 248 959 B1 can completely block the dangerous UV-B region and block the UV-A region by more than two-thirds. The UV protection of such a coating is usually in the range of ≥ 46%, preferably ≥ 85%, particularly preferably ≥ 98%, very particularly preferably ≥ 99%.

A particularly high UV protection, especially for photochemically very sensitive active ingredients is achieved when the transmission for wavelengths in the visible wavelength range between 380 nm and 420 nm is less than 50%. Will only radiation in the UV-B range, d. H. blocked for wavelengths smaller than 380 nm, so no sufficient protection for photochemically sensitive materials is achieved.

Such UV protective layers can be used in sol-gel technology, by means of dipping, spin-on, Drain or capillary technique may be applied. Alternatively, however, they can also be applied by means of cathode sputtering, by sputtering, by physical high-vacuum vapor deposition, also ion or plasma-assisted or by chemical vapor deposition, also plasma-assisted by microwave application or by spray pyrolysis. The number of single layers can vary from one to more than 7 layers. For example, 4-layer systems are widely used in the sputtering industry. All of these technologies can provide thin glasses for the realization of the described invention.

Additionally or alternatively, the thin glass panes are coated on the outside facing away from the active ingredient with an IR-reflecting layer to the active ingredient against damaging IR radiation in the spectral range of 780 nm to 1 mm, in particular in the spectral range of 780 nm to 50 microns, and thus to protect a dangerous temperature entry.

According to the invention, such an IR-reflecting coating contains a silver layer (Ag layer). In addition to this Ag layer, further layers are necessary for adhesion promotion, as oxidation protection for the Ag layer, for antireflection coating for the Ag layer and also as sacrificial layer for a tempering process, so that a complete layer package results for such an IR-reflecting coating. In order to increase the IR reflection of such a coating, a layer package with 2 Ag layers is preferably built up. The Ag layers have a layer thickness of 5 to 20 nm, preferably 10 to 15 nm.

Such a layer system comprises, for example, a cover layer, consisting for example of a Bi oxide, SnO ₂ , TiO ₂ , ZnO or Si ₃ N ₄ , a subsequent blocking layer of z. B. NiCr or partially oxidic Al, Ti, Zn, Pb of the following silver layer and a blocking layer arranged under the silver layer and an adhesive layer, the z. B. from a Bi oxide, SnO ₂ , TiO ₂ , ZnO, Si ₃ N ₄ consists. The adhesive layer in turn then establishes contact with the thin glass pane. As described above, in the abovementioned layer system, the cover and adhesive layer act as a protective layer of the silver layer and as an adhesion promoter between the glass surface and the silver layer. They also ensure that the silver layers grow up homogeneously. Such a layer system is very detailed in Hans-Joachim Gläser, "Thin Film Technology on Flat Glass", pages 167-171 , described. The relevant disclosure is included in the application in full. Such an IR-reflecting coating can be applied, for example, with a magnetron sputtering method.

Thermal barrier coatings based on silver coating systems are referred to as "soft coatings". As an alternative to silver layer systems, so-called "hard coatings" can also be used as thermal barrier coatings. The term "hard-coating" is understood to mean layer systems which comprise transparent layers based on semiconductors. Essentially, these are semiconducting layers of the materials indium oxide (In ₂ O ₃ ), tin oxide (SnO ₂ ) and zinc oxide (ZnO). These materials are also referred to as TCOs (Transparent Conductive Oxides). Such layer systems are for example in Hans-Joachim Gläser "Thin Film Technology on Flat Glass", pages 155-164 , described in detail. The relevant disclosure is included in the application in full. Of particular importance as a thermal barrier coating have been obtained based on SnO ₂ : F. Such thermal barrier coatings, based on SnO ₂ : F coatings, are now produced using CVD technology. If such layer structures based on SnO ₂ : F are applied to a thin glass, the layer system comprises a diffusion barrier layer, for example of SiOx (CH) y. The "hard coatings" comprising, for example, a SnO ₂ : F layer, have a high chemical resistance and a high and secure adhesion.

The thin glass panes may also carry a colored or opaque coating on the outside facing away from the active substance in order to reduce or prevent the entry of harmful electromagnetic waves in the visible spectral range from 380 nm to 780 nm. Such a coating may also be a reflective metal layer.

In one embodiment of the invention, the thin-glass panes of the cavity consist of an alkali-free glass in order, in particular in the case of chemically sensitive substances, to avoid a diffusion of alkalis into an active substance. Such a thin glass is, for example, the alkali-free thin glass AF 45 from Schott AG or the alkali- and arsenic-free aluminum silicate thin glass AF 37 from Schott AG.

Other glasses which can be used are, for example, virtually alkali-free aluminum silicate thin glasses, alkali-reduced soda-lime thin glasses or also a borosilicate thin glass, such as the D 263 from Schott AG.

To such a cavity as active ingredient packaging for a sheet-like application, such. B. to be able to use an active ingredient patch, this is formed according to the invention surface. Under a surface-shaped cavity is a planar expansion of the cavity at the same time understood significantly lower thickness. In this case, in one embodiment, the surface may be flat.

In another embodiment, one or both or further thin glass panes is curved or edged to form the cavity or cavities. The curved or edged shape can extend over the entire surface of the thin glass panes or even over only a part of the surface in the form of one or more elevations. To form such formations, the thin-glass panes are heated accordingly and partially formed in a sinking mold.

In this case, in a further embodiment of the invention, a plurality of cavities can also be produced side by side. This is particularly advantageous if only a portion of the active ingredient should be releasable for delivery.

As a particularly advantageous embodiment, the cavity is formed from two thin glass panes, which are connected together at their edge and form at least one cavity between them. It can also be formed several cavities by correspondingly many thin glass panes arranged one above the other and formed at the edges together form a corresponding number of cavities. The cavities are then arranged one above the other. This is z. B. advantageous if a larger amount of active ingredient to be provided without the cavity of a cavity would have to be designed too large.

Another application where two or more cavities are provided is the packaging of two or more component materials. The activation takes place after opening the cavities by breaking and then mixing the components by flowing or diffusing into each other.

The cavity is produced in one embodiment of the invention by a spacing of the respective two thin glass panes by a correspondingly defined thickness of the sealing frame. The sealing frame connects the thin glass panes circumferentially around the cavity. The seal may be an adhesive, or a self or UV curing or thermally curable, optionally fine glass powder contained material.

For the application of the seal on a thin glass pane, for example, the screen printing method is used or the application by means of material dispensers, so-called dispenser. In one exemplary method, the still soft seals are first precured in a drying oven before the thin glass panes are assembled together into a cavity. During assembly, the two processed thin glass panes are aligned with each other and combined to form a panel. The position of the two glass plates to each other is determined by UV-curing Polymerfixierpunkte.

After mounting the two glass plates to form a cavity, the complete curing of the seals takes place in a hot pressing furnace. This must be done under pressure to ensure that the seal thickness is exactly equal to the thickness of the cavity and that the pre-calculated cavity volume for the active ingredient is achieved with small tolerances.

In this case, a panel can contain a single or a multiplicity of cavities which are separated from each other by sealing frames. After curing of the sealing material, the then stable cavities are separated by scribing and breaking. The break edges are ground round.

As an alternative to connecting the thin glass panes with a seal, the panes can also be fused together to form the cavity. This can be done by means of the conventional flame method, as is known to the person skilled in the art for ampoules. In a preheating step, the cavity is preheated up to 800 ° C. To close the edge area is heated up to 1400 ° C, so that the touching outer edges of the thin glass panes merge together. A flame spreads the heat and surrounds the entire edge area of the cavity. There is a homogeneous heating. For this reason, slightly lower voltages occur in the glass in the case of the flame than in the case of a laser fusion.

However, the laser method is preferred. Compared to a flame, the heat is introduced more concentrated by the laser beam. The energy input is greatest in the center of the entry site at the edge of the cavity (90%) and decreases towards the inside (10%). The continuous rotation of the cavity causes a uniform heating of the glass.

On the other hand, the laser can bring the energy for heating much faster into the glass. This is a significant advantage because the environment is less heated and so the filled active ingredient is not thermally stressed so high. The required energy for preheating and fusing the edges of a cavity is generated for example by a CO2 laser. At a wavelength of 10.6 mm, the laser beam is almost completely absorbed by the glass, with normal incidence into the glass results in an absorption of over 90%. The CO2 laser can be a dual-beam decoupling which allows to control the preheating and closing independently. The non-contact machining of the cavities by laser technology guarantees the highest possible protection against particles that could cause flames. As a result, the laser system meets the requirements of the pharmaceutical industry, especially with regard to sterility.

A fusion technique is particularly advantageous for extremely sensitive active ingredients, since there are no other contact materials, such as a seal.

Depending on the filling technique, a small opening for filling the cavity with the active ingredient, which is subsequently closed, may remain in the connecting seam in both cases.

In one embodiment of the invention, spacers can be provided in the cavity, which predetermine the spacing of the two thin-glass panes and stabilize the glass panes relative to one another. The spacers can, depending on the compatibility with the active ingredient, consist of small glass or plastic beads. These are fixed to individual evenly distributed over the surface points before mounting the thin glass panes on at least one disc.

The spacing of the thin glass panes for forming cavities is usually in the range from 10 to 2000 μm, preferably in the range from 30 to 500 μm.

The filling of the cavity can be done by a vacuum method, similar to the filling of LCD display glass. The still empty cavity is placed in a vacuum chamber so that it is above the drug fluid. Then the chamber and thus also the empty cavity is evacuated. The cavity is then immersed in the active substance liquid with the filling hole in advance, and then the chamber is filled again with air or an inert gas, for example nitrogen. Atmospheric pressure forces the active ingredient into the cavity. In a further process step, the filling hole is closed.

For economic production, several cavities can also be filled in a glass composite. Subsequently, a separation takes place by mutual scribing and breaking.

Alternatively, the filling through a small matching opening in the peripheral seal of the thin glasses with the aid of z. B. a cannula. Subsequently, the opening is closed by means of a sealing compound, such as a self or UV-curing or curable, possibly fine glass powder contained material.

To deliver the drug, the cavity is broken. This happens mainly by kinking or impressions of the cavity. In order to bring about a targeted break, at least one thin glass pane may contain predetermined breaking points. These can be z. B. be introduced by scratches or previous damage, for example by means of a laser.

In one embodiment of the invention, this is a single targeted predetermined breaking surface, so that the active ingredient can escape from the cavity only after a break at the predetermined breaking point by a crack. This is advantageous for a very low dosage of the active ingredient in the delivery or even for active ingredients that react strongly with atmospheric oxygen. Here, a large part of the active substance can still remain in the protective cavity during delivery.

In another embodiment of the invention, this involves a high number of specific predetermined breaking points, which can be arranged as a matrix, so that the active substance can emerge from the cavity distributed over a surface area at break points at the predetermined breaking points. This is advantageous to assist in distributing the drug in the donor area adjacent to the cavity.

In order to control a breakage of the thin glasses for delivering an active substance from the cavity, the thin glasses according to the invention have a wall thickness of 20 to 1100 μm, preferably 30 to 100 μm, particularly preferably 30 to 70 μm.

In a further embodiment of the invention, the thin glasses are thermally or chemically prestressed, that when the cavity breaks, it breaks up into as many small individual pieces as possible and thus the active substance can emerge distributed over the surface as evenly as possible.

In a particularly preferred embodiment of the invention, an active substance reservoir of an absorbent matrix for receiving and controlled delivery of the active substance adjoins the cavity. If the cavity is broken open to deliver the active ingredient, the active ingredient diffuses into the active substance reservoir and is released from there. The drug reservoir contains a matrix which is suitable for taking up the active ingredient and metering it in quantity and time.

Such a matrix may be in the form of a sponge, a fleece or a cotton wool. In particular, a drug reservoir consists of a water-insoluble polymer matrix of a base polymer and conventional additives. The Selection of the base polymer depends on the chemical and physical properties of the active ingredient (s) used. Base materials are, for example, polymers such as rubber, rubber-like synthetic homopolymers, copolymers or block polymers, polyacrylic acid esters and their copolymers, polyurethanes, copolymers of ethylene, polyisobutylene, polybutylene and polysiloxanes and silicones. In principle, all polymers are suitable which are substantially insoluble in water and, depending on the application of the active ingredient packaging in direct and indirect contact with the skin, have no adverse effects on humans.

The type of additives depends on the polymer used and the active ingredient. Depending on their function, additives can be classified into plasticizers, absorption promoters, carriers, stabilizers or fillers. The physiologically acceptable substances which are suitable for this purpose are known to the person skilled in the art.

On the other hand, the active substance reservoir reliably retains the fragments of the cavity after they have broken open and prevents them from entering the environment. It may be for the retention of glass splinters in addition z. B. reinforced by a nylon fabric.

For further delivery of the active substance, in one embodiment of the invention, an active substance reservoir for the targeted delivery of the active substance can furthermore adjoin a membrane which is permeable to the active substance. This may in particular be a microporous membrane. The strength, number of pores and / or size of the pores can be adjusted for the application and the active ingredient to determine the passage rate of the drug through the microporous membrane.

Alternatively, the membrane may also be provided instead of the drug reservoir. The membrane is then designed so that it reliably retains the fragments of the cavity after it breaks up and prevents them from entering the environment. It can be used to restrain glass splinters additionally z. B. reinforced by a nylon fabric.

As materials for such a membrane are polyethylene, polyamide, ethylene-vinyl acetate copolymers, but also filled with low molecular weight porous layers are conventional and known in the art.

In a further embodiment of the invention, an impermeable cover layer is applied to the sides which are not intended to give off any active ingredient in the application. Such a cover layer is impermeable to the active substance and opaque to protect it, in order to ensure the effectiveness of the active substance after opening of the cavity, before it could be deactivated by environmental influences. Such a cover layer may be composed of any suitable material, in particular of plastic polymers. For example, it may be made from one or more materials, such as polyester, polyurethane, polyethylene, polyethylene terephthalate, polypropylene, and polyvinylchloride materials. The side of the cover layer which does not face the cavity may also preferably be lacquered with a lacquer containing epoxy resins or polyaminoamide resins containing opacifiers. Thus, the cover layer may be a cloudy or transparent material, preferably a transparent polyester material such as a polyethylene terephthalate (PET). However, such a cover layer can also be made of a metal foil, such as an aluminum foil, coated alone or with a polymeric substrate. It can also be used textile fabrics, if the active ingredient or the components of the drug reservoir can not pass through the textile material due to their physical nature. In a preferred embodiment, the topcoat is a composite that provides overall strength to the drug patch and serves as a barrier to loss of drug. In addition, aluminum-coated foils or composites are also suitable.

In a preferred embodiment of the invention, the active substance reservoir and / or the permeable membrane and / or the cover layer forms a shell into which the cavity can be inserted. This makes it possible, on the one hand, for the means for delivering the active substance to be storable and transportable separately from the active substance in the cavity. On the other hand, it is made possible that the cavity can only be selected with the appropriate active substance before application and then introduced into a suitable sheath for use. Cavity with active ingredient and shell can thus be brought together optimized for the application in each case. Also, after delivery of the active ingredient from a cavity, another cavity with active ingredient can be introduced into the envelope and opened so that the envelope can be used several times in succession and the delivery of active substance from several cavities in succession is made possible.

In another embodiment of the invention, the drug is not free in the cavity, but in the cavity, a drug reservoir in the form of a matrix is provided, which receives the active ingredient in the cavity and releases controlled after opening the cavity. As a rule, it is then possible to dispense with an active substance reservoir adjacent to an outer surface of the cavity. For the release of the active ingredient in this embodiment, one for the Active substance permeable membrane attached to at least one surface of the cavity.

This alone or together with a cover layer, the fragments of the cavity, after breaking up, reliably back and prevents them from entering the environment. It can be used to restrain glass splinters additionally z. B. reinforced by a nylon fabric.

In principle, all suitable materials can be used as the material for such a matrix which absorbs the active substance. In particular, water-soluble or water-swellable polymers can be used. Among these are exemplified: polyvinyl alcohol and its copolymers, polyvinylpyrrolidone and its copolymers, polyethylene glycols, preferably having a molecular weight of about 1000 daltons, which are thus solid at room temperature. Other readily applicable polymers are alginates, pullulan, guar gum with gum arabic or other vegetable lumens, cellulose, in particular microcrystalline cellulose and its derivatives such. As methylcellulose, hydroxyethylcellulose, hydroxymethylpropylcellulose, etc., but also other carbohydrates such. As starch, particularly preferably in derivatized or modified form. However, peptidic polymers such as collagen and gelatin may also be considered. Water-soluble and water-swellable polymers have the advantage that they do not suddenly become more ductile and more diffuse when water is absorbed, and thus release the entrapped active ingredient more uniformly. This is particularly useful in applications in which the dispersed drug is to be included only gradually in the drug delivery process. If a faster transition is preferred, molecular, water-soluble substances are to be used advantageously as sole or mixed auxiliaries for the construction of the matrix. First and foremost, because of their property of forming glassy solidifying, diffusion-resistant particles, sugars and their derivatives come into consideration, primarily sucrose, glucose, lactose, fructose, but also sugar alcohols, such as sorbitol or mannitol. In principle, all pharmaceutically compatible water-soluble substances, which have the property of liquefying under a water vapor tension of about 98 percent relative humidity (as provided by the skin), such as. As sodium chloride, urea, malic acid or citric acid. Additives to achieve known in the art further functionalities such. As stabilizers (especially antioxidants), fillers, but also micellar modifiers (lecithins) can be provided according to the respective requirement.

Depending on the intended use of the active ingredient packaging, in one embodiment of the invention, a pressure-sensitive adhesive layer is additionally attached. Depending on the type of active ingredient packaging, this may be located below the permeable membrane, below the active substance reservoir or directly on the cavity. The pressure-sensitive adhesive layer can be applied over the entire surface and in this case is permeable to the active substance. But it can also be attached only in an edge region of the delivery area for the active ingredient.

The control of the drug transfer from the drug package to the receiving surface can be done via a metering membrane. which has a property controlling the active ingredient to the skin or can moderate the too rapid absorption of moisture from the skin.

The role of dosing membrane can also be taken over by the pressure-sensitive adhesive layer. Such a pressure-sensitive adhesive layer consists of a pressure-sensitive adhesive which is suitable for use e.g. B. is physiologically harmless as a transdermal patch and for the or the active ingredient (s) is permeable. Examples of such pressure-sensitive adhesives are highly diffusible lipophilic polymers, such as. As polysiloxanes and acrylate copolymers.

In order to achieve the desired initial release of the active ingredient in the application, it may be necessary to load this pressure-sensitive adhesive layer with active ingredient already during production.

To ensure transport and storage, the pressure-sensitive adhesive layer is covered with a removable protective layer, such as a release liner, which is stripped off before delivery of the active ingredient. Suitable for transdermal systems. Release films are made of z. Polyester, polyethylene terephthalate, polyethylene, polypropylene or polyvinyl chloride films or composite films (inter alia paper / polyethylene). They belong to the state of the art and can be taken from this. The release liner may be provided with a release coating, for example it may be siliconized or fluorosilicated. The release liner may have a protruding end that helps it peel off the patch more easily.

Such cavities as active ingredient packaging can be used in many ways. A particularly preferred application is in a transdermal patch. Using two thin glass panes, which are joined together at a defined distance, a cavity is produced. This cavity is filled with the active ingredient.

The cavity is incorporated into a plaster by covering it on the skin side with an absorbent fleece as active substance reservoir, which in turn is coated or surrounded on the skin side with a pressure-sensitive adhesive layer. The pressure-sensitive adhesive layer is for the Cover transport and storage with a peelable protective film. The pressure-sensitive adhesive layer can cover the entire surface facing the skin and in this case is permeable to active substance. The disadvantage is that not all pressure-sensitive adhesives are suitable and also compatible with active ingredients. Since the fleece remains free from the active substance in the transport and storage state and is infiltrated with the active substance only immediately before use, it is a great advantage of the solution according to the invention that the pressure-sensitive adhesive need only be applied to the fleece in a peripheral region and the fleece in direct skin contact can deliver the drug. As a result, all skin-compatible pressure-sensitive adhesive can be selected and in the drug delivery to the skin, the pressure-sensitive adhesive material need not be considered.

To the side facing away from the skin, the cavity is covered with an active substance-impermeable cover layer. The drug is protected during the storage of the patch through the glass packaging from environmental influences, similar to an ampoule packaging. In the application, the glass cavity is broken by bending the patch, the active ingredient is absorbed by the fleece and can be delivered to the skin. It should be noted that thin glasses in the specified thickness range break very good natured due to the low mechanical stresses. The protective effect of the fleece and the cover layer is completely sufficient to safely avoid any risk to the user due to cuts.

Such a drug package offers z. B. as a pharmaceutical packaging a comparable protective effect and chemical resistance as a glass vial, a glass ampoule, glass carpous or glass syringe.

Another use of the invention is the active ingredient packaging for fragrances z. B. as an advertising insert in magazines or for distribution to exhibitions. Between two thin glass panes with a thickness in the range of 50 microns to 100 microns, filled with the perfume drug reservoir z. B. in the form of an absorbent nonwoven or paper. Subsequently, the thin glasses are glued together to produce the cavity. Alternatively, the cavity can also be filled with the fragrance later. For protection from the fragments of the cavity after opening by breaking, the cavity is surrounded by a perfume-permeable membrane. In this case, the permeable membrane may also be a closable shell, in which the cavity is introduced at any time. The fragrance is protected during storage by the glass packaging from environmental influences and in turn can not diffuse out of the package similar to a glass perfume bottle. In the application, the cavity is opened by kinking, and the fragrance diffuses through the permeable membrane to the user. The protective effect of the permeable membrane is completely sufficient to safely avoid any danger to the user due to cuts.

Furthermore, the invention can be used for the packaging of chemical indicator solutions. For example, here the active ingredient is a color indicator for the presence of a gas, such. B. be oxygen. In this case, the active ingredient could be a redox color indicator which, after opening the cavity, is taken up by a drug reservoir in the form of an absorbent nonwoven. About the color change of the web, the presence or absence of the gas can be detected.

Another use is the use of the invention to build very long storable electric batteries, which are usually carried as backup batteries and activated only in use, such. B. batteries for emergency signal lamps.

A reaction partner of the battery is stored in the cavity separately from the other active ingredients. In this case, however, the other active ingredients can be stored in a separate cavity or cavities. If the cavities are opened by breaking open, the reactants come together and the battery can release its energy. In storage, the active ingredients remain protected against environmental influences, so that a long shelf life of the battery can be guaranteed for more than 20 years.

A design of such a battery consists of a magnesium alloy as an anode and a sintered silver chloride as a cathode. The battery can be activated with water. To protect the components from the unwanted ingress of moisture during storage, they are enclosed in a glass cavity. Other examples are types of lithium batteries, which can only be activated if required with a storage time of more than 20 years.

Another use is the storage of two- and multi-component systems.

For example, several cavities each contain components of a multi-component adhesive, for example one epoxy resin and one hardener each. The cavities are brought between two surfaces to be joined and opened by the pressure of the surfaces on each other, so that the components of the adhesive can mix, harden and connect the surfaces together. The Fragments of the thin glass cavity act in the glue joint, like a glass powder, stabilizing.

Detailed description of the drawings

The invention will be described below with reference to the example and the drawing 1 be described in more detail.

1 shows schematically an embodiment of a transdermal patch 1 , Using two alkali-free thin-glass panes 21 . 22 with a thickness in the range of 30 microns to 50 microns, which are connected at a distance of 100 to 300 microns together, a cavity is produced. The connection is made by a glass powder-containing adhesive, which for the cavity as a seal 3 between the thin glass plates acts. In order to define the distance between the two thin glass panes, spacers in the form of glass spheres corresponding to the selected diameter are fixed at a plurality of, preferably four points of a thin glass pane distributed over the surface. To fill the cavity, an opening, not shown, is provided in the seal. The cavity is now using a vacuum process with the drug 4 filled and closed the opening with the adhesive containing a glass powder. The cavity is incorporated into a plaster by bringing it to the skin side with an absorbent fleece 5 is covered. To the side facing away from the skin is the cavity of a drug-impermeable cover layer 8th covered. The skin is the fleece 5 surrounding the top layer with a pressure-sensitive adhesive layer 6 coated. The pressure-sensitive adhesive layer is for transport and storage with a peelable protective film 7 covering, with the protective film 7 at the same time the fleece 5 covered. In the application, the glass cavity 2 broken by kinking the patch, the active ingredient is absorbed by the fleece and can be delivered to the skin. This is the protective film 7 removed and fixed the patch with the pressure-sensitive adhesive layer on the skin. It should be noted that thin glasses in the specified thickness range break very good natured due to the low mechanical stresses. The protective effect of the fleece and the cover layer is completely sufficient to safely avoid any risk to the user due to cuts.

It is understood that the invention is not limited to a combination of the features described above, but that the skilled person will arbitrarily combine all the features of the invention, as far as is expedient.

LIST OF REFERENCE NUMBERS

1

Transdermal patch

2

cavity

21

First thin glass pane

22

Second thin glass pane

3

poetry

4

active substance

5

fleece

6

Adhesive layer

7

releasable sheet

8th

topcoat

QUOTES INCLUDE IN THE DESCRIPTION

This list of the documents listed by the applicant has been generated automatically and is included solely for the better information of the reader. The list is not part of the German patent or utility model application. The DPMA assumes no liability for any errors or omissions.

Cited patent literature

• DE 3315272 [0004]
• DE 2135533 [0005]
• DE 19912623 [0009, 0010]
• WO 91/09731 [0012]
• DE 3650575 [0013]
• US 5008110 [0014]
• EP 1248959 B1 [0030, 0031]

Cited non-patent literature

• Hans-Joachim Gläser, "Thin Film Technology on Flat Glass", pages 167-171 [0036]
• Hans-Joachim Gläser "Thin Film Technology on Flat Glass", pages 155-164 [0037]

Claims (25)

Active substance packaging for dispensing active ingredients comprising at least one surface-impermeable thin-glass cavity, in which an active substance is contained, and which is designed such that it can be broken open to dispense the active ingredient. Active ingredient packaging according to claim 1, wherein the cavity has a wall thickness of 20 to 1100 μm, preferably 30 to 100 μm, particularly preferably 30 to 70 μm. Active ingredient packaging according to claim 1 or 2, wherein the cavity is formed of a largely alkali-free thin glass. Active ingredient packaging according to one of the preceding claims, wherein the cavity is formed from a colored thin glass, in particular a brown glass. Active ingredient packaging according to one of the preceding claims, wherein the inner wall of the cavity is coated with a barrier layer, in particular of silicon dioxide. Active ingredient packaging according to one of the preceding claims, wherein one of the thin glass surfaces, in particular the surface forming the outer wall of the cavity, is coated with a UV-reflecting coating. Active ingredient packaging according to one of the preceding claims, wherein one of the thin glass surfaces, in particular the surface forming the outer wall of the cavity, is coated with an IR-reflecting coating. Active ingredient package according to one of the preceding claims, wherein one of the thin glass surfaces, in particular the surface forming the outer wall of the cavity, is coated with a coating which reflects electromagnetic waves in the spectrum of visible light. Active substance packaging according to one of the preceding claims, wherein the cavity is formed from two thin glasses, which are connected to one another with a sealing frame or fused together. Active ingredient packaging according to one of the preceding claims, wherein the cavity is formed of thin glasses and one or both thin glasses are partially lowered for the formation of the cavity. Active ingredient packaging according to one of the preceding claims, wherein at least two cavities are arranged in multiple layers one above the other. Active ingredient packaging according to one of the preceding claims, wherein the cavity is breakable by buckling or by pressing the active ingredient packaging. Active ingredient packaging according to one of the preceding claims, wherein at least one thin glass pane of the cavity has a predetermined breaking point. The active ingredient package according to any of the preceding claims, wherein the active ingredient package further comprises an active agent reservoir of an absorbent matrix for receiving and controlled delivery of the active ingredient, and the drug reservoir adjoins the at least one surface of the cavity. Active ingredient packaging according to one of the preceding claims, wherein the active substance package for targeted delivery of the active substance further comprises a permeable membrane for the active substance. The active ingredient package according to any one of claims 1 to 13, wherein the drug package further comprises an active agent reservoir of absorbent matrix for receiving and controlled delivery of drugs and the drug reservoir is enclosed in at least one cavity and a drug permeable membrane on at least one surface of the cavity this adjoins. The active ingredient package of any one of the preceding claims, wherein the drug package further comprises a drug impermeable cover layer. Active substance package according to one of claims 14, 15 or 17, wherein it is designed such that the drug reservoir and / or the permeable membrane and / or the cover layer form a shell into which the cavity is insertable. The active ingredient package according to any of the preceding claims, wherein the active ingredient package further comprises a pressure-sensitive adhesive layer. Active ingredient packaging according to one of the preceding claims, wherein the active substance package further comprises a removable protective layer (release film). Active ingredient packaging according to one of the preceding claims, wherein the active ingredient package is an active ingredient patch, preferably a transdermal patch. Use of a drug package according to any one of claims 1 to 20 for the encapsulation of fragrances. Use of an active substance package according to one of Claims 1 to 20 for the encapsulation of chemical indicators. Use of an active substance package according to one of Claims 1 to 20 for the storage of two- or multi-component materials. Use of a drug package according to any one of claims 1 to 20 for the storage of batteries such as batteries for emergency signal lamps.

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