JP2010254618A - Carnitine and glycyrrhizic acid-containing oral solid agent - Google Patents

Abstract

<P>PROBLEM TO BE SOLVED: To provide an oral solid agent which contains carnitine or a salt thereof and glycyrrhizic acid or a salt thereof, and in which the reduction of the content of the glycyrrhizic acid or the salt thereof is suppressed. <P>SOLUTION: The oral solid agent includes carnitine or a salt thereof, a pH regulator, and glycyrrhizic acid or a salt thereof. Aminoacetic acid, dried aluminum hydroxide gel, magnesium aluminosilicate, magnesium silicate, synthetic aluminum silicate, synthetic hydrotalcite, magnesium oxide, dihydroxyaluminum aminoacetate, magnesia alumina hydrate, aluminum hydroxide-sodium bicarbonate coprecipitation product, aluminum hydroxide-magnesium carbonate mixed dried gel and the like are cited as preferable concrete examples of the pH regulator. <P>COPYRIGHT: (C)2011,JPO&INPIT

Description

  The present invention relates to an oral solid preparation containing carnitine or a salt thereof and glycyrrhizic acid or a salt thereof.

  Carnitine is a kind of organic acid that exists in the body, and it is said that it plays a role as a carrier that carries free fatty acids into the mitochondria, which is the site of oxidation. It is used as a supplement. In addition, it has gastric acid secretion promoting action, gastric peristaltic movement enhancing action, and gastric circulatory blood flow volume increasing action, so it is used to alleviate symptoms such as loss of appetite and gastrointestinal tract function (Non-Patent Document 1, etc.).

  Glycyrrhizic acid has anti-inflammatory action, anti-allergic action, gastric mucosal proliferating action, ulcer repair action and the like, and is used as an anti-allergic agent and gastrointestinal drug. It is also known as the main component of licorice (Non-Patent Document 2 and others).

By the way, as an oral preparation containing carnitine and glycyrrhizic acid, an oral liquid preparation that stably maintains glycyrrhizic acid in an acidic liquid preparation containing carnitine and a thickening polysaccharide is known (Patent Document 1).
However, in oral solid preparations containing carnitine or a salt thereof and glycyrrhizic acid or a salt thereof, it has not been known so far that a problem arises in the content stability of glycyrrhizic acid or a salt thereof in the oral solid preparation.

JP 2004-175672 A

OTC Handbook 2008-09 Pages 505-506 Academic Information Distribution Center Co., Ltd. OTC Handbook 2008-09 Pages 370-371 Academic Information Distribution Center Co., Ltd.

The present inventor first conducted various studies on the properties of carnitine or a salt thereof and an oral solid preparation containing glycyrrhizic acid or a salt thereof. Surprisingly, when glycyrrhizic acid and carnitine contact each other, glycyrrhizic acid or its It was found that the content of salt over time decreases.
Accordingly, an object of the present invention is to provide carnitine or a salt thereof, and an oral solid preparation containing glycyrrhizic acid or a salt thereof, in which a decrease in the content of glycyrrhizic acid or a salt thereof in the oral solid preparation is suppressed.

  Therefore, the present inventor diligently studied to solve the above problems, and by adding a pH regulator to carnitine or a salt thereof, and glycyrrhizic acid or a salt thereof, the content of glycyrrhizic acid or a salt thereof is reduced. It has been found that a suppressed oral solid preparation can be obtained.

  That is, the present invention provides an oral solid preparation containing carnitine or a salt thereof, a pH adjuster, and glycyrrhizic acid or a salt thereof.

According to the present invention, in an oral solid preparation containing carnitine or a salt thereof and glycyrrhizic acid or a salt thereof, an oral solid preparation in which a decrease in the content of glycyrrhizic acid or a salt thereof is suppressed can be provided.
Moreover, without passing through a complicated process, manufacturing the oral solid agent by which the fall of the content of glycyrrhizic acid or its salt in the oral solid agent containing carnitine or its salt and glycyrrhizic acid or its salt was suppressed was manufactured. it can.

Carnitine or a salt thereof used in the present invention includes carnitine itself and a pharmaceutically acceptable salt of carnitine. Since carnitine has an asymmetric carbon, an optical isomer exists, but in the present invention, any of D isomer and L isomer of optical isomers and a mixture thereof may be used.
Specific examples of carnitine or a salt thereof include carnitine, levocarnitine, carnitine chloride, levocarnitine chloride, carnitine tartrate, levocarnitine tartrate, carnitine fumarate, levocarnitine fumarate, and the like. Particularly preferred, one or more of these may be used. These are known compounds and may be produced by known methods, or commercially available products may be used.

  The content of carnitine or a salt thereof in the oral solid preparation of the present invention may be determined by appropriate examination according to the sex, age, symptom, etc. of the user, but there is an amount that can be taken from 15 to 1500 mg per day. The amount that can be taken is preferably 30 to 750 mg.

The glycyrrhizic acid or a salt thereof used in the present invention includes glycyrrhizic acid itself and a pharmaceutically acceptable salt of glycyrrhizic acid.
Specific examples of glycyrrhizic acid or a salt thereof include glycyrrhizic acid, dipotassium glycyrrhizinate, monoammonium glycyrrhizinate, diammonium glycyrrhizinate, disodium glycyrrhizinate, trisodium glycyrrhizinate, and the like. Potassium and monoammonium glycyrrhizinate are preferred, and one or more of these may be used. These are known compounds and may be produced by known methods, or commercially available products may be used.

As the glycyrrhizic acid or a salt thereof, licorice (licorice) or licorice extract containing glycyrrhizic acid or a salt thereof as a component can also be used.
The licorice refers to the roots and strons of Glycyrrhiza uralensis F., Glycyrrhiza glabra L. or other related genera as described in the 15th Amendment Japanese Pharmacopoeia. As licorice, in addition to roots and strons, whole plants, leaves, stems, bark, branches, corolla, petals, flower buds, seeds, fruits, etc. of the above-mentioned plants are cut as they are, or cut into pieces or pieces or powders. It can be used by grinding. The powder of licorice is called “licorice powder”.

  In addition, as the licorice extract used in the present invention, a solution obtained by adding a suitable leaching agent to a licorice having an appropriate size and leached, and further a solution obtained by concentrating the leaching solution (crucian licorice extract, licorice extract, licorice tincture) In addition, a leaching solution or a solution obtained by concentrating the leaching solution and solidified by drying or the like (licorice extract powder, dried licorice extract) is also included. In addition, the said concentration etc. can be performed by the well-known method as described in 15th revision Japanese Pharmacopoeia preparation general rules.

  Examples of the leaching agent include lower monohydric alcohols such as methanol, ethanol and n-butanol; lower polyhydric alcohols such as ethylene glycol, propylene glycol, 1,3-butylene glycol and glycerin; ethers such as diethyl ether; Ketones such as acetone and ethyl methyl ketone; esters such as ethyl acetate; halogenoalkanes such as dichloromethane and chloroform; aromatic hydrocarbons such as benzene and toluene; and water. These may be used alone or in combination of two or more. Furthermore, the extract can be dried.

  In the present invention, when licorice is used as glycyrrhizic acid or a salt thereof, it is preferable to use licorice powder, licorice extract, licorice crude extract, licorice dry extract, or licorice extract powder. As described above, these may be produced by a known method, or commercially available products may be used.

  The content of glycyrrhizic acid or a salt thereof in the oral solid preparation of the present invention may be determined by appropriate examination according to the sex, age, symptoms, etc. of the user. The amount that can be taken 1 to 400 mg is preferred, the amount that can be taken 0.5 to 200 mg is more preferred, and the amount that can be taken 5 to 200 mg is more preferred.

  The compounding ratio of carnitine or a salt thereof and glycyrrhizic acid or a salt thereof contained in the oral solid preparation of the present invention may be appropriately determined and determined according to the daily dose of each component. Or it contains 2-60 mass parts of carnitine or its salt with respect to 1 mass part of the salt (glycyrrhizic acid conversion), and what contains 4-30 mass parts is more preferable.

  The pH adjuster used in the present invention can be used as a pharmaceutical itself or as an additive suitable for food or oral administration as long as it exhibits the effects of the present invention or has sufficient qualities to solve the problems. All of these should be included, but basic compounds are preferred, those having a pH of 6.5 or more when the oral solid preparation is made into a 10% by mass aqueous solution or aqueous suspension are more preferred, and the pH is Those having a pH of 7 or more are more preferred, and those having a pH of 8 or more are particularly preferred. The pH of the 10% by mass aqueous solution or water suspension is preferably 10 or less.

Preferred specific examples of the pH adjuster include aminoacetic acid, L-arginine, dry aluminum hydroxide gel, dry sodium carbonate, sodium citrate hydrate, magnesium aluminate silicate, calcium silicate, magnesium silicate, Synthetic aluminum silicate, synthetic aluminum silicate / hydroxypropyl starch / crystalline cellulose, synthetic hydrotalcite, disodium succinate hexahydrate, magnesium oxide, dihydroxyaluminum aminoacetate, DL-sodium tartrate, sodium L-tartrate, water Alumina magnesium oxide, aluminum hydroxide gel, aluminum hydroxide / sodium bicarbonate coprecipitation product, aluminum hydroxide / magnesium carbonate mixed dry gel, aluminum hydroxide / magnesium carbonate / calcium carbonate coprecipitation Composition, potassium hydroxide, sodium hydroxide, magnesium hydroxide, sodium bicarbonate, potassium carbonate, calcium carbonate, potassium bicarbonate, sodium carbonate hydrate, magnesium carbonate, precipitated calcium carbonate, precipitated magnesium carbonate, copper chlorophyllin potassium, Copper chlorophyllin sodium, calcium pantothenate, tetrasodium pyrophosphate, bentonite, sodium polyacrylate, anhydrous sodium pyrophosphate, anhydrous sodium monohydrogen phosphate, anhydrous calcium hydrogen phosphate, meglumine, magnesium aluminate metasilicate, 5'-ribo Examples thereof include, but are not limited to, nucleotide disodium, trisodium phosphate, calcium hydrogen phosphate, sodium hydrogen phosphate hydrate, and the like. Moreover, these may be individual and may combine 2 or more types.
Of these, aminoacetic acid, dry aluminum hydroxide gel, magnesium aluminate silicate, magnesium silicate, synthetic aluminum silicate, synthetic hydrotalcite, magnesium oxide, dihydroxyaluminum aminoacetate, magnesium alumina hydroxide, hydroxylation Aluminum / sodium bicarbonate coprecipitation product, aluminum hydroxide / magnesium carbonate mixed dry gel, aluminum hydroxide / magnesium carbonate / calcium carbonate coprecipitation product, magnesium hydroxide, sodium bicarbonate, magnesium carbonate, precipitated magnesium carbonate, anhydrous Calcium hydrogen phosphate, magnesium aluminate metasilicate, and calcium hydrogen phosphate are preferred.

The content of the pH adjusting agent in the oral solid preparation of the present invention is the mixing ratio and content of carnitine or its salt and glycyrrhizic acid or its salt according to the daily dose, especially the oral solid preparation Depending on the content of carnitine or a salt thereof contained therein, it may be appropriately determined and determined, but the pH of a 10% by mass aqueous solution or aqueous suspension of the oral solid preparation of the present invention is 6.5 or more. It is preferable to mix so that the pH is 7 or more, and it is particularly preferable to mix so that the pH is 8. The pH of the 10% by mass aqueous solution or water suspension is preferably 10 or less.
In order to adjust the pH to 6.5 or more, the pH regulator is usually preferably contained in an amount of 2 to 100 parts by mass with respect to 1 part by mass of carnitine. Those are more preferred.

  The oral solid preparation of the present invention may contain components other than carnitine or a salt thereof, a pH adjuster, and glycyrrhizic acid or a salt thereof. The component is not particularly limited, but preferably has an effect or an effect on gastrointestinal diseases, such as a mucosal repair agent, analgesic and antispasmodic agent, gastric agent, digestive agent, intestinal regulating agent, antipruritic agent, antifoaming agent, etc. These may be used alone or in combination of two or more.

  Examples of the mucosal repairing agent include sodium azulenesulfonate, aldioxa, L-glutamine, gefarnate, sucralfate, histidine hydrochloride, porcine gastric wall pepsin degradation product, porcine gastric wall acid hydrolyzate, methylmethionine sulfonium chloride, red bud, engosac and the like.

  Analgesic and antispasmodic agents include oxyphencyclimine hydrochloride, dicyclomine hydrochloride, methixene hydrochloride, scopolamine hydrobromide, methyl atropine bromide, methyl anisotropine bromide, methyl scopolamine bromide, methyl-1-hyostiamine bromide, bromide Parasympathetic blockers such as methylbenactidium, belladonna extract, isopropamide iodide, diphenylpiperidinomethyldioxolane iodide, funnel extract, funnel root total alkaloid citrate; antispasmodic agents such as papaverine hydrochloride; ethyl aminobenzoate, etc. Local anesthetics; herbal medicines such as peonies.

  Examples of stomachic agents include aniseed fruit, aloe, fennel, turmeric, cormorant, life-prolonging grass, cormorant, cormorant, cormorant root, dry husk, chaff, pheasant, keihi, gentian, kojin, koboku, goshuyu , Cucumber, colombo, conzurango, salamander, yamana, shisoshi, shukusha, shrimp, shrimp, green peel, mint, stone root, centaurium grass, burdock root, red clover, sweet potato, daikon scented, daisou, chikutsujinjin, choji, chimpi , Capsicum, spruce, animal gall, oyster, nutmeg, carrot, mint, japonica, hops, homica extract, sleepy leaves, mokko, yakchi, yutan, ryutan, ryukyo, fennel oil, cinnamon oil, ginger oil, ginger oil Oil, cho Bethanechol chloride, gastrointestinal function modifiers such as trimebutine maleate; di oil, spruce oil, peppermint oil, lemon oil, l-menthol, crude drug dl- menthol dry yeast and the like.

  Digestive agents include starch digestive enzymes, protein digestive enzymes, fat digestive enzymes, fibrin digestive enzymes, complex digestive enzymes, etc .; Ursodeoxycholic acid, oxycorates, cholic acid, bile powder, bile extract And bile extract powder, dehydrocholic acid, and animal gallbladder.

  Examples of the intestinal regulating agent include herbal medicines such as asenyaku, ubai, kujin, ketsumeishi and gennoshouko; live intestinal bacteria such as lactic acid bacteria and natto bacteria.

Antifungal agents include bactericides such as acrinol, berberine chloride, guaiacol, creosote, phenyl salicylate, guaiacol carbonate, berberine tannate; bismuth subsalicylate, bismuth nitrate, bismuth carbonate, bismuth subgallate, tannic acid, tannin Examples include astringents such as acid albumin and methylenethymol tannin; adsorbents such as kaolin, hydroxynaphthoic acid aluminum, pectin, and medicinal charcoal; coating agents such as calcium lactate; herbal medicines such as quintuplet, hawthorn, and yam; and loperamide hydrochloride.
Examples of the antifoaming agent include dimethylpolysiloxane.

  The oral solid preparation of the present invention can be produced and formulated based on a known method described in the 15th revised Japanese Pharmacopoeia General Rules for Preparations. Examples of the dosage form of the oral solid preparation include tablets, powders, granules, fine granules, pills, capsules (excluding liquid-filled capsules) and the like.

In addition, as an oral solid preparation, carnitine or a salt thereof and glycyrrhizic acid or a salt thereof in the solid preparation are contained so that they do not substantially come into contact with each other, and a pH adjuster is further added. An oral solid preparation produced and formulated is more preferred.
The above “carnitine or a salt thereof and glycyrrhizic acid or a salt thereof so as not to substantially contact each other” means glycyrrhizin resulting from contact between carnitine or a salt thereof and glycyrrhizic acid or a salt thereof in a preparation It means that they are contained so that they do not come into contact with each other to the extent that a decrease in the content of the acid or its salt is suppressed.

  Such a preparation prepared by blending so as not to substantially contact each other can be easily understood by a general pharmaceutical technology researcher. Based on a known method, a preparation additive is appropriately added. Can be manufactured and formulated. Specifically, the following (i) to (f) can be exemplified as the form of the oral solid preparation, and these can be produced and formulated by known methods.

(I) A powder or granule produced by granulating any one of carnitine or a salt thereof and glycyrrhizic acid or a salt thereof by an appropriate method, and mixing the other without granulation. In addition, a preparation in which the granular material is further coated by an appropriate method. In addition, a pH adjuster may be mix | blended in a granular material and may be mix | blended separately from a granular material.
(B) Carnitine or a salt thereof, and glycyrrhizic acid or a salt thereof are granulated to form a granular material, a powder or a granule prepared by blending these, and a preparation in which the granular material is further coated by an appropriate method. . In addition, a pH adjuster may be mix | blended in any one granular material, may be mix | blended in both granular materials, and may be mix | blended separately from these granular materials.
(C) A capsule filled with the powder or granule prepared in (i) or (b) above.
(D) Tablets obtained by tableting the granular material produced in (i) or (b) above.
(E) A multilayer tablet prepared so that carnitine or a salt thereof and glycyrrhizic acid or a salt thereof do not contact each other, and a preparation in which the multilayer tablet is further coated by an appropriate method. As the multilayer tablet, carnitine or a salt thereof, and glycyrrhizic acid or a salt thereof are preferably located in different layers. As a multilayer tablet of three or more layers, a layer containing carnitine or a salt thereof and glycyrrhizic acid or a salt thereof More preferably, the salt-containing layers are positioned so as not to contact each other. In addition, the granular material manufactured by said (i) and (b) can be used as carnitine or its salt, and glycyrrhizic acid or its salt. Moreover, in the said multilayer tablet, a pH adjuster may be located in one layer, and may be located in two or more different layers.
(F) A dry-coated tablet in which any one of carnitine or a salt thereof and glycyrrhizic acid or a salt thereof is arranged in a nuclear tablet, and a preparation in which the dry-coated tablet is further coated by an appropriate method. As carnitine or a salt thereof, and glycyrrhizic acid or a salt thereof, the granular material produced in (i) or (b) above can be used. In the dry coated tablet, the pH adjuster may be located in the dry tablet, may be located in the outer shell, or may be separately located in either the dry tablet or the outer shell.

In the oral solid preparation of the present invention, one or more additives for preparation may be used as necessary. Examples of the formulation additive include an excipient, a binder, a disintegrant, a lubricant, a coloring agent, and a corrigent.
Examples of the excipient include lactose, starches, crystalline cellulose, sucrose, mannitol, xylitol, and light anhydrous silicic acid.
Examples of the binder include hydroxypropylmethylcellulose, hydroxypropylcellulose, gelatin, pregelatinized starch, polyvinylpyrrolidone, polyvinyl alcohol, pullulan and the like.
Examples of the disintegrant include carmellose, carmellose calcium, croscarmellose sodium, crospovidone, corn starch, and low-substituted hydroxypropylcellulose.
Examples of the lubricant include magnesium stearate and talc.
Examples of the colorant include tar pigments and iron sesquioxide.
Examples of the corrigent include stevia and aspartame.

The oral solid preparation of the present invention can be taken 1 to 4 times per day before meals, between meals, after meals, before going to bed.
In addition, since the oral solid preparation of the present invention contains carnitine or a salt thereof and glycyrrhizic acid or a salt thereof, anorexia, decreased appetite, stomach / abdominal fullness, indigestion, stomach weakness, overeating, overeating, It has efficacy and effects on overdrinking, overdrinking, heartburn, leaning, stomach upset, chest gripping, scalding, vomiting, etc., and is useful as a pharmaceutical, quasi-drug, and other health foods.

  EXAMPLES The present invention will be described in detail below with reference to examples, but the present invention is not limited to these examples.

Comparative Example 1
216.0 g of carnitine chloride, 126.0 g of licorice extract powder (manufactured by Nippon Powder Chemical Co., Ltd.), 176.4 g of hydroxypropylcellulose, 351.0 g of carmellose calcium, and 2640.6 g of D-mannitol were mixed with a high-speed stirring granulator (vertical granulator (Later: manufactured by POWREC). Ethanol was added to this mixture and kneaded to obtain a kneaded product. This kneaded product was granulated with an extrusion granulator (pellet: manufactured by Dalton) with a screen, and the granulated product was further dried with a fluidized bed dryer (flow coater: manufactured by Freund). The dried product was sized using a sizing machine (speed mill: manufactured by Okada Seiko Co., Ltd.) equipped with a screen and then classified using a sieve to obtain granules.

Example 1
216.0 g of carnitine chloride, 120.0 g of licorice extract powder (manufactured by Nippon Powder Chemical Co., Ltd.), 176.4 g of hydroxypropylcellulose, 351.0 g of carmellose calcium, 2640.6 g of D-mannitol, 234.0 g of synthetic hydrotalcite, 234.0 g of dry aluminum hydroxide gel and 234.0 g of magnesium hydroxide were mixed with a high-speed stirring granulator (vertical granulator: manufactured by POWREC). Ethanol was added to this mixture and kneaded to obtain a kneaded product. This kneaded product was granulated with an extrusion granulator (pellet: manufactured by Dalton) with a screen, and the granulated product was further dried with a fluidized bed dryer (flow coater: manufactured by Freund). The dried product was sized with a sizing machine (speed mill: manufactured by Okada Seiko Co., Ltd.) equipped with a screen and then classified using a sieve to obtain granules.

Example 2
216.0 g of carnitine chloride, 120.0 g of licorice extract powder (manufactured by Nippon Powder Chemical Co., Ltd.), 176.4 g of hydroxypropylcellulose, 351.0 g of carmellose calcium, 2640.6 g of D-mannitol, 1170.0 g of synthetic hydrotalcite, 1170.0 g of dried aluminum hydroxide gel and 1170.0 g of magnesium hydroxide were mixed with a high-speed stirring granulator (vertical granulator: manufactured by POWREC). Ethanol was added to this mixture and kneaded to obtain a kneaded product. This kneaded product was granulated with an extrusion granulator (pellet: manufactured by Dalton) with a screen, and the granulated product was further dried with a fluidized bed dryer (flow coater: manufactured by Freund). The dried product was sized with a sizing machine (speed mill: manufactured by Okada Seiko Co., Ltd.) equipped with a screen and then classified using a sieve to obtain granules.

Test Example 1 pH measurement Comparative Example 1, Examples 1 and 2 were each added with 10 mL of water to 1.0 g to prepare a suspension. A pH meter (in accordance with the pH measurement method of the 15th revised Japanese Pharmacopoeia) The pH was measured with HORIBA, Ltd., model: F-55. The results are shown in Table 1.

Test Example 2 Content Stability Test Each granule of Comparative Example 1, Example 1 and 2 was stored at 50 ° C. for 1 month, and after storage at 60 ° C. for 1 week, and then taken out. Each pharmaceutical product in the 15th revised Japanese Pharmacopoeia The content of glycyrrhizic acid was measured according to the licorice quantitative method.
That is, the content stability was compared from the peak area of glycyrrhizic acid of each specimen. The results are shown in Table 1.

As is apparent from Table 1, carnitine or a salt thereof, and an oral solid preparation containing glycyrrhizic acid or a salt thereof, which contains a pH adjuster, stabilizes the glycyrrhizic acid or the salt in the oral solid preparation. It has been found that it exhibits excellent effects.
In addition, from the above results, carnitine or a salt thereof, and glycyrrhizic acid or a salt thereof are blended so that they do not substantially come into contact with each other, and an oral solid preparation containing a pH adjuster exhibits a more excellent effect. I understand things.

Claims (4)

  An oral solid preparation containing carnitine or a salt thereof, a pH adjuster, and glycyrrhizic acid or a salt thereof.   The oral solid preparation according to claim 1, comprising carnitine or a salt thereof and glycyrrhizic acid or a salt thereof so as not to substantially contact each other.   The oral solid preparation according to claim 1 or 2, which contains a granular material containing carnitine or a salt thereof and / or a granular material containing glycyrrhizic acid or a salt thereof.   The oral solid preparation according to any one of claims 1 to 3, which has a pH of 6.5 or more when a 10 mass% aqueous solution or water suspension is prepared.