DE102005059606A1 - Active agent-application device for application in a gastro-intestinal tract, in a bladder or in uterus, comprises application mechanism with the agent, and a holding mechanism for the application mechanism - Google Patents

Abstract

The active agent-application device (1) for application in a gastro-intestinal tract, in a bladder or in uterus, comprises application mechanism (2) loaded with the agent, and a holding mechanism (6) for the application mechanism. The holding mechanism holds the application mechanism in a normal position as long as the mechanism is in an application position and enables to displace the application mechanism of the application position into delivery position of the agent. In the delivery position, the mechanism exhibits a typical cross section extending. The active agent-application device (1) for application in a gastro-intestinal tract, in a bladder or in uterus, comprises application mechanism (2) loaded with the agent, and a holding mechanism (6) for the application mechanism. The holding mechanism holds the application mechanism in a normal position as long as the mechanism is in an application position and enables to displace the mechanism of the application position into delivery position of the agent. In the delivery position, the mechanism exhibits a typical cross section extending, which is 5-times of a minimum cross section extending in the application position. The mechanism is formed in such a way that it stands in connection with less than 5% of the interior wall area of the target organ, in the delivery position. The Application mechanism in the delivery position is present as net, whose maximal interior volume is larger than the interior volume of a target organ of the gastro-intestinal tract. A light width of meshes of the net is half of a largest organ-inlet opening of the target organ. The Application mechanism in the delivery position is present as spiral, whose maximum cross section extending is larger than the interior cross section of the target organ. The distance between adjoining windings of the spiral is a multiple diameter of a single strand developing the spiral. The mechanism is formed from mucoadhesive-single strand, which has rectangular cross section and which is carried out by multilayers. One of the layers of the single strand exhibits an active substance and a function material different from the active substance. The application mechanism is formed in such a way that in the delivery position, a central section of an interior lumen of the target organ is kept free.

Description

The The present invention relates to a drug delivery device for use in a large volume Target organ, namely in the gastrointestinal tract, in the urinary bladder or in the uterus, according to the preamble of the claim 1.

Such a drug delivery device for use in the stomach is known from US 5,002,772 A , Such application devices are known as gastro-retentive systems, which are also referred to below as GRS. These are systems that linger in the stomach and are not promoted by the gastric peristalsis. With regard to the body compatibility, the known application device is still in need of improvement.

It is therefore an object of the invention, an active ingredient application device of the type mentioned in such a way that their body compatibility is improved.

These The object is achieved by an application device with the in the characterizing part of the claim 1 specified characteristics.

According to the invention was recognized that compatibility issues in the generic application device stir, therefore that there in the central portion of the inner lumen of the target organ the drug carrier is arranged in the form of a tablet. This increases the resistance of the application device z. B. against liquid, which the target organ between a junction in the target organ and an outlet from the target organ passes, considerably. This resistance often solves body's own defense reactions, z. As by peristaltic contraction movements, which is undesirable. Due to the inventive design the applicator device such that the central portion of the Inner lumen of the target organ is kept, becomes the resistance in the target organ opposite z. B. a liquid passage significantly reduced, so that the compatibility is improved. The Danger of endogenous defense reactions is thereby reduced. At the same time, advantages of the known remain Applikationsvorrichtung, with the small contact surface at the Inner wall of the target organ in the delivery position of the applicator related, receive. Due to this small inner contact surface results in a low Irritation of the target organ, so that also here body-own defense reactions be avoided. This represents an advantage of the embodiment according to the invention across from other known application devices that as bubbles or balloons cover the inner wall of the target organ almost completely. The retention device can in the application device according to the invention be integrated into the applicator. This is special then the case when the applicator device of a material with shape memory (Memory material) is constructed. Alternatively, it is possible to have one separate restraint in the form of z. As a capsule to provide, which is the applicator in the rest position or the applicator device otherwise prevents it from going to the delivery position. Instead of a Capsule may also be a tablet, a dragee or a suppository provided be. The retention device can z. B. as tough Be formed mass in which the applicator in the Resting position is stored. An example of such a tough mass is paraffin. For example, instead of a paraffin a gel or a fat can be used. The device according to the invention is designed such that it targeted into the target organ can be introduced, at the same time a safe and long-lasting Linger in the desired Target organ is achieved. In the delivery position, the application device clothes the inner wall of the target organ partially off, with only a small Part of the inner wall actually covered by the applicator device. Before application in the Target organ is the application device in the insertion position before, in which the applicator device with respect to the dispensing position in particular collapsed or compressed. In the Einbringstellung is a targeted introduction the applicator device in the target organ, for example by oral administration, possible. After application, d. H. Reaching the desired target organ, that goes Applicator device in the delivery position via. This puts the Applicator at least partially to the inner wall of the target organ at. In the application device according to the invention In particular, the risk of gastric obstruction is not given. In addition, the risk is reduced that the applicator through z. B. by the target organ continuous liquid undesirable from the Target organ is transported out.

contact portions The applicator device according to claim 2 are to achieve a high body tolerance especially suitable.

An applicator device in the form of a network according to claim 3 ensures at low volume in the insertion position a large maximum umspannbares inner volume in the delivery position. Such an applicator can therefore be present in the Einbringstellung strongly compressed, so that z. B. an oral intake is facilitated. On the other hand, a relatively large target organ can be almost completely lined by the mesh, so that a uniform drug delivery is given by the applicator to the inner wall of the target organ. The mesh size of the network ensures that the network is through occurs from z. B. liquid from an orifice into the target organ towards an orifice from the target organ at most a minimal resistance, e.g. B. opposed by a leg laying over the respective organ openings strand. Preferably, the mesh size of the mesh is the same size as the largest organ opening of the target organ or even larger. Examples of organ openings are the cardia or the pylorus when used in the stomach. The net can be in the form of an ordered net or also as a disordered knit.

A Applicator device as a helix according to claim 4 can be with relatively little production effort from a single strand finished. The maximum cross-sectional extension of the coil ensures a safe investment of the outside the helix on the inner wall of the target organ in the delivery position the applicator device.

there introduces distance ratio according to claim 5 to an advantageously low percentage coverage the inner wall of the target organ with the applicator device, what again leads to a low risk of an endogenous defense reaction.

A Single-strand design of the applicator device according to claim 6 can be produced with very little effort. Such a single strand can especially without bias as flabby thread-like strand be formed, which is in the delivery position of the applicator statistically applied to the inner wall of the target organ. Such Applicator device is particularly simple.

The Single strands from which the applicator devices according to claims 3 to 6 are constructed have a typical diameter between 1 micron and 2 mm, advantageous from 50 μm to 1 mm, particularly advantageous from 200 microns to 0.5 mm. Especially advantageous is the execution the single strands as microfibers. Such a single strand design of the applicator device In particular, it can be designed to be so flexible and yielding that the applicator means a peristaltic movement of the target organ can follow, which is an undesirable Next promotion prevents the applicator.

One Single strand according to claim 7 may be designed in particular strip-shaped. Non-rotationally symmetric single-strand cross-sections can then, if a limp single strand without shape memory is used, too an advantageous and approximately uniform lining of the inner wall of the target organ. Alternatively it is natural also possible, single strands to provide with a round cross-section.

One Multilayered single strand according to claim 8 leads to an advantageously increased design freedom for the Applicator. The different layers that make up the Single strand is built up, can fulfill different functions, z. B. in connection with the control of the transition between the Einbringstellung in the delivery position, with the release of active ingredient or with others Functions.

at an execution According to claim 9, at least one of the layers as far as possible executed drug-free be, wherein a further layer contains at least one active ingredient. In the Use as a dosage form in human medicine or veterinary medicine As a result, too high a local concentration of the active ingredient tissue side avoided. In this case, the tissue side will largely be executed without active ingredient.

Advantageous come here from 1 to 10 layers are used, particularly advantageous 2 to 7, more preferably 2 to 4 layers. In the embodiment according to claim 10 can the different layers take over different functions, to ensure a controlled release of active ingredients. For example, can It may be beneficial to quickly break through an active ingredient release through a second layer a constant release over one longer Provide period and through a third layer of active ingredient directly to the tissue of the application organ, e.g. to give the stomach. Alternatively, by such a layer structure and the time staggered delivery of different drugs possible if these are present in different layers containing the respective active ingredient only deliver after the previous shift has been used there Released drug. Another alternative is the use of layers with substances that accelerate the degradation of the device. So, after complete drug release then be achieved that these substances targeted a fast Allow removal of the device which minimizes irritation of the affected target organ. Through a Such a multi-layer structure is in particular a pulsed release of active ingredient possible.

A Another option is that a multi-layered construction also incorporation of color-coded layers allowed what the product labeling and recognizability when used on the patient. In order to can prevent accidental ingestion by patients and Overall, patient compliance will be increased.

In a further embodiment of the invention can be largely dispensed with the embedding, wherein the first form of the structure before application is autostable. By action triggered by an external factor, for example, by temperature or pH or light, the structure can go into its second form. Materials having the property of adopting two stable forms, one of which may be converted to the second form by external influence, are known to those skilled in the art and are referred to as shape memory materials. These may be metals but in particular polymers, such as polylactides or polyglycosides or polyurethanes which have the appropriate properties.

factors the one form return trigger, can while humidity, temperature (-50 ° C to 200 ° C, preferably 0 ° C to 50 ° C, especially advantageously 30 ° C up to 45 ° C), Light advantageous in the wavelength range between 200 and 800 nm, particularly advantageous between 250 and 500 nm, or the presence of ions, in particular biologically relevant ions such as hydronium ions, calcium, sodium or magnesium ions be.

at the pH parameter as the triggering factor Advantageously, a range of 1 to 13 is used, especially advantageously between 1 and 8, very particularly advantageously from 1, 2 to 4.

Conceivable are also factors that indirectly trigger the direct factors. Conceivable Here is, for example, ultrasound, which generate heat in the body in question can.

The used materials can be metals or metal alloys, but especially plastics, wherein advantageously thermoplastic elastomers (TPE) can be used.

The Systems usually consist of a composite of at least two Materials of different glass transition temperatures of the hard segment and the switching segment / soft segment.

The permanent form of the materials results from melting above the temperature of the hard segment and then cooling below the temperature of the hard segment, but above the transition temperature of the switching segment / soft segment. The polymer is now brought into its temporary form (deformation), by cooling down below the transition temperature of the Switching segment / soft segment can be fixed. The process of programming, using temperature as an external trigger takes place as follows: Is the temperature higher than the transition temperature of the switching segment, these segments are flexible and the polymer can be elastically deformed. The temporary shape is created by cooling below the transition temperature the switching segments fixed. When the polymer is reheated, turn off the permanent, original Shape again.

Especially biodegradable and / or biocompatible polymers are advantageous used, such as polylactate or polyglycosides. In health care In particular, such systems are synthesized by the synthesis of macrodiols from the monomers such as L, L-dilactide, diglycolide, p-dioxanone, e-caprolactone, built up g-butyrolactone.

Farther can as additional Components water-soluble or largely water-soluble Polymers, such as modified celluloses (hydroxypropylmethylcellulose (HPMC), hydroxypropylcellulose (HPC), sodium carboxymethylcellulose (NaCMC)), and modified starches, or polysaccharides as well as other water-soluble polymers such as polyvinyl alcohol (PVA) can be used advantageously. Depending on the requirement can be advantageous also combinations of suitable materials can be used, wherein the materials used in different strand sections can be used and / or as a mixture, dispersed or dissolved.

Furthermore the material may contain further constituents such as plasticizers, dyes, Fillers and Stabilizers included. These other ingredients will ever as needed and under consideration of the desired Purpose of use selected. The expert can use the usual Access ingredients, which are disclosed in general knowledge. Alternatively, suitable ingredients under recourse on information from usual Reference works selected become.

Polymeric ingredients may include: polyvinyl alcohol (PVA), cellulose derivatives such as hydroxypropylmethylcellulose (HPMC), hydroxypropylcellulose (HPC), sodium carboxymethylcellulose (NaCMC), methylcellulose (MC), hydroxyethylcellulose (HEC), hydroxypropylethylcellulose (HPEC), starch and derivatives thereof, gelatins, Polyvinylpyrrolidone (PVP), gum arabic, pullulan, or acrylates. In addition, inter alia, the following auxiliaries may be included: fillers such as silica (SiO ₂ ), dyes such as chiolin yellow or titanium dioxide (TiO ₂ ), disintegrants or wicking agents such as Aerosil, emulsifiers such as Tween, Brij, plasticizers such as polyethylene glycol (PEG), propanediol or glycerin, preservatives such as sorbic acid or its salts.

The inventive device can the following, later also show structure described in detail with reference to FIG.

First, simple single-layer devices, ie devices that are essentially Made of only one material, conceivable. In this case, for example, one of the abovementioned materials forms a desired device, for example in the form of a strand which comprises the desired active substance, in addition to the principal material of the device which serves as a carrier for the active substance.

Furthermore is the use of different polymers or polymer blends in the above-described simple structure or in different layers a strand possible, what is called a laminate structure. In particular, the latter Laminate structure is advantageous in many applications because so that the properties of the device are targeted and easily modified can. So can For example, the rate of drug release the device, the degradation characteristics of the device or else the adsorption properties and thus the compatibility of the device in be adjusted specifically to a physiological environment.

Of the according to the invention to the Target agent to be delivered drug in a manner known in principle in the device according to the invention be introduced. In this case, the active ingredient dissolved as a dispersion or suspension be incorporated in the material used. It is also conceivable that the Active substance on the carrier structure represented by the structure superficial bound or adhered is. Here, the active substance, for example, nanoparticulate or in Embedded nanoparticles present.

The Delivery of active ingredients can be as a diffusion from a largely insoluble Matrix done and / or by decomposition of the active ingredient-containing layer. The degradation of a layer can take several hours, for example 2 to 24 h, advantageously 5 to 24 h, particularly advantageously 10 to 24 h, or several days, for example 1 to 30 d, advantageous 1 to 7 d, particularly advantageously 1 to 3 d, need.

For some Applications are dismantling times of several months adjustable, or Systems that are largely non-degradable to provide.

in this connection can different layers advantageously different disintegration times exhibit.

Furthermore is in a special embodiment the invention accommodates the active ingredient in a separate delivery system, which connected to the deployable structure in a suitable form is. Conceivable here are forms such as tablets, capsules, dragees or other, known in the art drug delivery systems. In this embodiment is achieved by the device according to the invention the anchoring of the whole system provided the drug delivery through the separate delivery system.

The Active substances which are for the application in the device according to the invention use can find basically include all orally administrable active ingredients, such as those in tablets, capsules or dragees.

in this connection can advantageously used all active ingredients of the following main groups are: weight loss / appetite suppressants, acidotherapeutics, analeptics / antihypoximics, Analgesics / antirheumatics, anthelminthics, antiallergic drugs, antianemics, antiarrhythmics, Antibiotics / anti-infectives, anti-dementia drugs (nootropics), antidiabetics, Antidotes, antiemetics / antivertiginosa, antiepileptics, antihemorrhagics (antifibrinolytics and other hemostats), Antihypertensives, antihypoglycemics, Antihypotonics, anticoagulants, antifungals, antiphlogistics, Antitussives, arteriosclerotic agents, beta receptors, calcium channel blockers, Inhibitors of the renin-angiotensin system, broncholytics / antiasthmatics, Cholagoga and bile duct therapeutics, cholinergics, corticoids (Internals), dermatological, diagnostic and diagnostic preparations, Diuretics, circulation-promoting Means, weaning, Agent for the treatment of addictions, enzyme inhibitors, preparations Enzyme deficiency and transport proteins, fibrinolytics, geriatrics, gout, Flu remedies and remedies for colds, gynecologics, hemorrhoids means (Proctologics), hepatics, hypnotics / sedatives, pituitary, hypothalamic hormones, other regulatory peptides and their inhibitors, immunomodulators, Cardiac, coronary, laxative, lipid-lowering, local anesthetics / neural therapeutics, Gastrointestinal, migraine, Muscle relaxants, anesthetics, neuropathic preparations and other neurotropic drugs Medications, ophthalmics, osteoporosis agents / calcium metabolism regulators, Parkinson's and other anti-extrapyramidal drugs, Psychotropic drugs, Rhinologics / Sinusitis agents, Roborantia / Tonics, Thyroid therapeutics, Sera, immunoglobulins and vaccines, sex hormones and their inhibitors, Spasmolytics / anticholinergics, platelet aggregation inhibitors, tuberculosis agents, Umstimmungsmittel, Urologika, Venentherapeutika, cytostatics.

alternative is also the use of diagnostics, such as contrast agents or markers possible, if by the device according to the invention a long-lasting release of such substances into investigative and diagnostic purposes is desired.

Depending on the use, in particular antimicrobial substances can be used. Markers are also conceivable.

The Production of the deployable component can be carried out by extrusion or coextrusion or punching or cutting out of web-shaped precursors. In this case, the person skilled in the art from the prior art To fall back on. The ones described in connection with the expandable pharmaceutical forms Manufacturing processes are suitable in principle for the production of Device according to the invention. The same applies to assembly, fixing of form 1 and introduction of active substances or excipients.

Further embodiments The invention will be described below with reference to the drawing. In this show:

1 a first embodiment of an active agent application device with a retaining device which holds an applicator device in a Einbringstellung;

2 the application device according to claim 1 during the displacement of the applicator device from the introduction position into the delivery position;

3 a section of a target organ using the example of the stomach in the region of the body and antrum with the applicator device in the delivery position;

4 an excerpt from 3 ;

5 an enlarged section of an inner wall of the target organ with the applicator in the dispensing position;

6 a further embodiment of an active agent application device with a retaining device which holds an applicator device in a Einbringstellung;

7 an instantaneous view during the introduction of the application device according to 6 into a target organ using the example of the intestine;

8th a further instantaneous view after introduction of the application device according to 6 into the target organ immediately after separation of the retaining device from the applicator device;

9 the applicator device of the application device according to 6 to 8th in the delivery position in the target organ;

10 the applicator after 9 at the drug delivery;

11 the applicator device according to 9 and 10 during their biodegradation; and

12 enlarged and very schematically different cross sections of single strands from which the application devices according to the 1 to 11 can be constructed.

The following is with reference to the 1 to 5 a first embodiment of a drug delivery device 1 described. This is for use in a target organ, in the present embodiment for use in the stomach. The drug delivery device has a deployable and drug loaded applicator device 2 in the form of a biodegradable single strands 3 . 4 built-up network. According to orientation of a network in a stomach single strands become 3 subsequently as longitudinal strands and the single strands 4 referred to as transverse strands. The single strands 3 . 4 limit between crossing points of the longitudinal strands 3 and the transverse strands 4 mesh 5 of the network. The clear mesh size of the mesh 5 is different than in the very schematic representation of the 3 to 5 , about half as large as a largest organ opening of the target organ, in the present case in about half the size of the diameter of the pylorus.

In addition to the applicator device 2 includes the drug delivery device 1 a retainer 6 in the form of a two halves 7 . 8th having capsule. In the in 1 shown rest position or storage form of drug delivery device 1 holds the retention device 6 the applicator device 2 in a Einbringstellung in which an oral intake of drug delivery device 1 is possible. In an operating position or final form of the active ingredient application device 1 allows the retention device 6 a displacement of the applicator device 2 in the Einbringstellung in one in the 3 to 5 shown delivery position. An intermediate position during deployment of the applicator device 2 in which the halves 7 . 8th the restraint device 6 have just separated is in 2 shown.

In the introduction position, the drug delivery device has 1 a minimum cross-sectional dimension Q _M corresponding to the cross-section of the retaining device 6 perpendicular to its longitudinal axis, of about 5 mm. In the dispensing position, the applicator device completely lines the stomach even where it has the largest circumference, so that a typical cross-sectional extension Q _{R of} the applicator device 2 in the delivery position of about 5 cm is present.

The single strands 3 . 4 have a diameter that is much smaller than the width of the mesh 5 , In the illustrated embodiment, the diameter of the single strands 3 . 4 about 1/10 of the mesh size. Due to this size ratio is the applicator 2 with about 1% of the inner wall surface of the target organ in contact. Due to the mesh size, the applicator device in the delivery position holds a central portion of an inner lumen 9 of the target organ free. This central section can therefore unhindered by z. B. liquid or crushed food will pass. Due to the mesh size, the applicator device 2 Also in the area of the cardia and the pylorus is no significant resistance to liquid or crushed food.

The Net can span a maximum of an internal volume, which is larger as the internal volume of the target organ, leaving a complete lining the inner wall of the target organ possible is.

The transition to the delivery position can be achieved by a bias of the applicator device 2 , by an at least partial embodiment of the applicator device 2 from shape memory material as well as by a mucoadhesion of the applicator device 2 or by any combination of the transient-bias / shape memory / mucoadhesion mechanisms of action. In particular, such a combination can be realized in the form of prestressing / mucoadhesion and in the form of shape memory / mucoadhesion. The mucoadhesion assists in that after the transition of the applicator device 2 in the delivery position this remains in place in the target organ.

4 shows schematically the release of active ingredient 9a from the single strands 3 . 4 into the target organ. Alternatively, a delivery can be made directly to the inner wall of the target organ.

The network of execution after the 1 to 5 is prepared as follows: First, a molding compound with integrated active ingredient is produced. The active ingredient may be dissolved, dispersed or adhered in the compound. Subsequently, the single strands 3 . 4 extruded. These are then called longitudinal strands 3 and transverse strands 4 aligned crosswise. At the crossing points the longitudinal strands become 3 with the cross strands 4 then glued. For gluing either an additional adhesive or bonding agent is used or it will be the respective single strands 3 . 4 for bonding at the crossing points selectively dissolved with subsequent removal of the solvent. As a further connection variant of the single strands 3 . 4 At the crossing points, it is possible to weld the individual strands together or to solder together. Subsequently, the net is brought into the form of a circular net by merging the ends of the existing after the alignment and bonding of the single strands surface network. Finally, the circular net is brought into the insertion position, ie into the retention device 6 used.

Another embodiment of a drug delivery device is described below with reference to 6 to 11 described. Components which correspond to those described above with reference to 1 to 5 have already been explained, bear the same reference numbers and will not be discussed again in detail. The 6 to 11 are not to scale insofar as that the cross section of the intestine compared to the cross section of the retention device 6 strongly understated. In fact, the cross section of the intestine is more than 5 times the minimum cross section of the retainer 6 ,

In the drug delivery device 10 after the 6 to 11 is an applicator device 11 as a single strand 12 built up. This lies in the in the 9 to 11 illustrated delivery position as a helix. The maximum cross-sectional extent of this helix is greater than an inner cross section of the target organ, in the present embodiment, larger than the inner cross section of the intestine. The helix is therefore located over the outer peripheral wall portions of the single strand 12 on the intestinal inner wall. The distance between adjacent turns of the helix is a multiple of the diameter of the single strand 12 , In the present case, the spacing of adjacent windings is about 7 to 8 times the diameter of the single strand 12 , This leads to that in the Abga order of the single strand 12 a maximum of 15% of the inner wall of the target organ touched.

7 shows the situation when inserting the drug delivery device 10 immediately before it reaches its destination in the target organ. 8th shows the application device 11 in the unfolded state, immediately after the capsule halves 7 . 8th have separated from each other. 10 shows the applicator 11 in the delivery position in the delivery of active ingredient 9a into the target organ. Alternatively, a direct delivery into the intestinal wall is possible. 11 shows the applicator 11 in advanced biodegradation.

12 shows schematically greatly enlarged different cross-sectional shapes of single strands, from which the applicator devices 2 or 11 can be constructed. A single strand 13 is as a two-layer laminate with a carrier layer 14 and a drug layer 15 executed. Overall, the single strand has 13 a roughly square cross-section. The active ingredient layer 15 has about one third of the thickness of the carrier layer 14 , In the carrier layer 14 it may be a prestressed layer in the insertion position or a shape memory layer. The carrier layer 14 may additionally contain another functional substance, eg. As a marker or a contrast agent. The single strand 13 can z. B. be prepared by co-extrusion or by a lamination process. In the production of the single strand 13 By coextrusion, it is possible to introduce this active ingredient in the context of the extrusion of the at least one layer to be loaded with active ingredient. This can be done by the active ingredient is dissolved or dispersed in the molding composition to be extruded.

A single strand 16 who is also in 12 is shown, is single-layered and also has an approximately square cross-section. The single strand 16 can z. B. be loaded evenly with active ingredient.

A single strand 17 in 12 otherwise the single strand 16 corresponds, has a round cross-section.

• a) Soweit der Schwerpunkt auf ein bioabbaubares Material gelegt wird, sind bevorzugte Materialvarianten eine Polylactidematrix, mit einem Weichmacher und als Wirkstoff z. B. einem Antibiotikum. Bei dem Antibiotikum kann es sich, z. B. zum Einsatz gegen Heliobacter Pylori, um ein Amoxicillin handeln.
• b) Soweit der Schwerpunkt auf eine mucoadhäsive Eigenschaft des Einzelstrang-Materials gelegt wird, kommt zum Einsatz eine Matrix aus Natriumcarboxymethylcellulose (NaCMC) mit einem Weichmacher und einem Wirkstoff, z. B. Amoxicillin.
• c) Soweit der Schwerpunkt auf die Eigenspannung des Einzelstrang-Materials gelegt wird, kommt zum Einsatz eine Matrix aus voll- oder teilkristallinem Polyvinylalkohol (PVA) mit einem Weichmacher und als Wirkstoff z. B. Amoxicillin.
• d) Als mehrschichtiges mucoadhäsives Einzelstrang-Material für den Einzelstrang 13 kommt zum Einsatz ein Laminat aus einerseits Natrium carboxymethuylcellulose (NaCMC) als mucoadhäsiver Schicht und andererseits Hydroxypropylmethylcellulose (HPMC) als wasserlöslicher Komponente mit einem Weichmacher und als Wirkstoff z. B. einem Antibiotikum. Die wasserlösliche Komponente löst sich während des Einsatzes des Einzelstrangs auf, sodass z. B. die NaCMC-Schichten nach Auflösen der HPMC-Schichten Wirkstoff abgeben können. Auch das NaCMC ist löslich, sodass ein Verbund NACMC und HPMC bioabbaubar ist.

The following material variants for the single strands 3 . 4 the execution after the 1 to 5 , for the single strand 12 the execution after the 6 to 11 as well as the single strands 13 . 16 . 17 according to the explanations 12 come used:

• a) As far as the focus is placed on a biodegradable material, preferred material variants are a polylactide matrix, with a plasticizer and as active ingredient z. B. an antibiotic. The antibiotic may be, for. For use against Heliobacter pylori, to act an amoxicillin.
• b) As far as the focus is on a mucoadhesive property of the single-stranded material, a matrix of sodium carboxymethylcellulose (NaCMC) with a plasticizer and an active ingredient, e.g. B. Amoxicillin.
• c) As far as the emphasis is placed on the residual stress of the single-strand material, comes to use a matrix of fully or partially crystalline polyvinyl alcohol (PVA) with a plasticizer and as active ingredient z. B. Amoxicillin.
• d) As a multilayer mucoadhesive single-stranded material for the single strand 13 a laminate of sodium carboxymethylcellulose (NaCMC) as a mucoadhesive layer and hydroxypropylmethylcellulose (HPMC) as a water-soluble component with a plasticizer and as an active ingredient, for example, is used. B. an antibiotic. The water-soluble component dissolves during use of the single strand, so z. B. the NaCMC layers can release drug after dissolution of the HPMC layers. Also the NaCMC is soluble, so that a composite NACMC and HPMC is biodegradable.

The drug delivery devices 1 . 10 can also be in another target organ, z. B. are used in the bladder. For this purpose, the drug delivery device 1 . 10 in the storage form z. B. introduced by means of a bladder catheter in the bladder. Subsequently, as described above, the transition of the applicator 2 . 11 in the delivery position in which it is held in the bladder.

In the illustrated embodiments of the application devices 1 . 10 becomes the displacement of the applicator device 2 . 11 from the introduction position into the delivery position triggered by a thermally induced opening of the retaining device 6 ,

The environment of such drug delivery devices 1 . 10 For use in large-volume target organs, which are often capable in particular of peristaltic contraction movements, is a significantly different than the environment of stents. In particular, the boundary condition that for the safe retention of the application device in the target organ this should be in contact with an inner wall portion of the target organ, requires a size difference of the applicator between the delivery position and the Einbringstellung, which is clearly beyond that, position and the Einbringstellung that clearly beyond that is what can be achieved with a stent.

Claims (10)

Active ingredient application device ( 1 ; 10 ) for use in a large-volume target organ, namely in the gastrointestinal tract, in the bladder or in the uterus, - with a deployable, loaded with drug applicator device ( 2 ; 11 ), - with a retaining device ( 6 ), - the application device ( 1 ; 10 ) holds in a rest position or storage form, as long as the applicator ( 2 ; 11 ) is in a Einbringstellung and - in an operating position or final shape of the application device ( 1 ; 10 ) a displacement of the applicator device ( 2 ; 11 ) from the introduction position into a delivery position, - wherein the applicator device ( 2 ; 11 ) is formed such that - in the dispensing position has a typical cross-sectional extension (Q _T ) which is at least 5 times a minimum cross-sectional extent (Q _M ) in the introduction position, - is in the dispensing position with less than 20% of an inner wall surface of the target organ in contact, characterized in that the applicator device ( 2 ; 11 ) is designed such that in the dispensing position, in particular, it has a central section of an inner lumen ( 9 ) of the target organ. Application device according to claim 1, characterized in that the applicator device ( 2 ; 11 ) is designed so that it is in the dispensing position with less than 10%, preferably less than 5% of the inner wall surface of the target organ in contact. Application device according to claim 1 or 2, characterized in that the applicator device ( 2 ) is in the delivery position as a network whose maximum umspannbares inner volume is greater than the inner volume of the target organ, wherein a clearance of mesh ( 5 ) of the network is at least half as large as a largest organ-orifice of the target organ. Application device according to claim 1 or 2, characterized in that the applicator device ( 11 ) is present in the delivery position as a helix whose maximum cross-sectional extension is greater than the internal cross-section of the target organ. Applikationsvorrichtung according to claim 4, characterized in that the distance between adjacent windings of the helix is a multiple of the diameter of a helix building single strand ( 12 ) is. Application device according to one of claims 1 to 5, characterized in that the applicator device ( 2 ; 11 ) from at least one, in particular mucoadhesive, single strand ( 3 . 4 ; 12 ; 13 ; 16 ; 17 ) is constructed. Application device according to claim 6, characterized in that the single strand ( 13 ; 16 ) has a non-rotationally symmetrical, in particular rectangular cross section. Application device according to claim 6 or 7, characterized in that the single strand ( 13 ) is multi-layered. Application device according to claim 8, characterized in that at least one ( 15 ) of the layers ( 14 . 15 ) of the single strand ( 13 ) has an active ingredient. Application device according to claim 9, characterized in that at least one ( 14 ) of the layers ( 14 . 15 ) of the single strand ( 13 ) has a different functional substance from the active ingredient.