JP7022420B2 - Oral composition - Google Patents

Description

The present invention relates to an oral composition comprising 3-hydroxy-3-methylbutyric acid or a salt thereof.

3-Hydroxy-3-methylbutyric acid (HMB) is a metabolic product of leucine, which is an essential amino acid, and is known to be involved in promoting muscle synthesis and suppressing decomposition. However, since the amount of HMB produced in the body is very small, attempts have been made to take this HMB as a supplement or the like.

Regarding such supplements, tablets containing 3-hydroxy-3-methylbutyrate calcium (HMBCa) and crystalline cellulose have been proposed (see Patent Document 1). In Patent Document 1, the tableting property is improved by using crystalline cellulose, and a tablet having no unevenness on the surface is obtained.

Japanese Unexamined Patent Publication No. 2015-218158

As mentioned above, HMB has been studied, but the effect of HMB and other components has not been studied much.

An object of the present invention is to provide an oral composition showing an excellent anti-obesity effect. Another object of the present invention is to provide an oral composition having an improved muscle-building effect of HMB.

As a result of diligent studies to solve the above problems, the present inventors have found that an excellent anti-obesity effect is exhibited by using a specific other material together with HMB or a salt thereof, and have completed the present invention. rice field. Further, they have found that the muscle-building effect of HMB or its salt can be improved by using a specific other material together with HMB or a salt thereof, and have completed the present invention.

That is, the present invention is as follows.
[1] It is characterized by containing 3-hydroxy-3-methylbutyric acid or a salt thereof, and at least one other material selected from ceramide, kudzu flower, reynoutria sachalinensis, kotsusaiho, musculoskeletal grass, and capsicum. Oral composition.
[2] The oral composition according to [1], which is an anti-obesity composition.
[3] The oral composition according to [1], which is a muscle-building composition.
[4] The oral composition according to [3], wherein the other material is at least one selected from ceramide and kudzu flower.

According to the present invention, it is possible to provide an oral composition showing an excellent anti-obesity effect. Further, it is possible to provide an oral composition having an improved muscle-building effect of HMB or a salt thereof. In particular, according to the present invention, it is possible to provide an oral composition exhibiting a more excellent anti-obesity effect and muscle-building effect when used in combination with exercise.

It is a figure which shows the evaluation result (the amount of lipid droplet per cell) of the differentiation | differentiation inhibitory effect of adipocyte when the composition (HMBCa + ceramide) of this invention is applied. It is a figure which shows the evaluation result (the amount of lipid droplet per cell) of the differentiation | differentiation inhibitory effect of adipocyte when the composition of this invention (HMBCa + kudzu flower) is applied. It is a figure which shows the evaluation result (the amount of lipid droplet per cell) of the differentiation | differentiation inhibitory effect of adipocyte when the composition of this invention (HMBCa + Reynoutria sachalinensis) is applied. It is a figure which shows the evaluation result (the amount of lipid droplet per cell) of the differentiation | differentiation inhibitory effect of adipocyte when the composition of this invention (HMBCa + Kotsusaiho) is applied. It is a figure which shows the evaluation result (the amount of lipid droplet per cell) of the differentiation | differentiation inhibitory effect of adipocyte when the composition of this invention (HMBCa + myobone grass) is applied. It is a figure which shows the evaluation result (the amount of lipid droplet per cell) of the differentiation | differentiation inhibitory effect of adipocyte when the composition of this invention (HMBCa + pearl oyster) is applied. It is a figure which shows the measurement result of the mRNA expression level of the Myogenin gene (myog) when the composition (HMBCa + ceramide) of this invention is applied. It is a figure which shows the measurement result of the mRNA expression level of the Myogenin gene (myog) when the composition of this invention (HMBCa + kudzu flower) is applied.

The oral composition of the present invention comprises 3-hydroxy-3-methylbutyric acid (HMB) or a salt thereof, and at least one other material selected from ceramide, kudzu flower, reynoutria sachalinensis, kotsusaiho, musculoskeletal grass, and pearl oyster. It is characterized by containing.

The other materials used together with HMB or a salt thereof may be used alone or in combination of two or more. When two or more other materials are used in combination, it is preferable to combine other materials having a high synergistic effect with HMB or its salt, and in the present invention, when used as a muscle-building composition, HMB or its salt or ceramide. And kudzu flower combination is preferable, and when used as an anti-obesity composition, a combination of two or more selected from HMB or a salt thereof and Reynoutria sachalinensis, Kotsusaiho, muscle bone grass, and Togarashi is preferable.

By using other materials together with HMB or a salt thereof, the differentiation of adipocytes is suppressed, whereby obesity can be suppressed. That is, the oral composition of the present invention can be used for anti-obesity, reduction of body fat, diet and the like.

Furthermore, by using at least one selected from ceramide and kudzu flower together with HMB or a salt thereof, the effect of HMB or a salt thereof can be improved. That is, the oral composition of the present invention can improve the muscle-building effect and the muscle fatigue recovery (muscle fatigue improving effect) effect of HMB or a salt thereof, and can improve the shape-up, muscle-building of athletes, and post-illness. It can be used for muscle recovery, prevention of sleeplessness in the elderly, suppression of muscle damage during exercise, recovery of muscle fatigue after exercise, improvement of basal metabolism, and the like.

[3-Hydroxy-3-methylbutyric acid or a salt thereof]
3-Hydroxy-3-methylbutyric acid (HMB) is a metabolite of the essential amino acid leucine and is synthesized in the human body. In the present invention, HMB or a salt thereof can be used. The salt of HMB is not particularly limited, and examples thereof include calcium salt, sodium salt, potassium salt, and magnesium salt, and calcium salt (HMBCa) is preferable from the viewpoint of muscle-building effect and anti-obesity effect. As the HMB or a salt thereof in the oral composition of the present invention, those synthesized by a known method or commercially available products can be used. The commercial product is not limited as long as it is applicable to food.

The content of 3-hydroxy-3-methylbutyric acid or a salt thereof is not particularly limited as long as it has a muscle-building effect and / or an anti-obesity effect, and is, for example, 0.1 to 99 with respect to the total amount of the composition. %, Preferably 1 to 98%, more preferably 5 to 97%.

[Other materials]
In the oral composition of the present invention, it is preferable to use at least one other material selected from ceramide, kudzu flower, reynoutria sachalinensis, kotsusaiho, musculoskeletal grass, and capsicum, together with HMB or a salt thereof.

(Ceramide)
The ceramide in the oral composition of the present invention includes human-type ceramides such as ceramide 1, ceramide 2, and ceramide 3, as well as animal-derived ceramides extracted from the brain and spinal cord of cows, horses, pigs, etc., wheat, rice, and the like. Plant-derived ceramides extracted from soybeans, spinach, corn, konjac, pineapple and the like can be used. Further, the ceramide in the oral composition of the present invention may be sugar ceramide, and specific examples thereof include those to which monosaccharides such as galactosylceramide and glucosylceramide are bound, and those to which oligosaccharides are bound. Can be done. In the oral composition of the present invention, it is preferable to use plant-derived ceramide, and it is more preferable to use glucosylceramide derived from gramineous plants such as wheat, corn, and rice, among which muscle-building effect and / or anti-ceramide is used. From the viewpoint of obesity effect, it is particularly preferable to use glucosylceramide extracted from rice or seeds collected from rice. Examples of the solvent used for extraction include water; lower alcohols such as ethanol, methanol, isopropanol and butanol; lower esters such as ethyl acetate and methyl acetate; acetone; a mixed solvent of these and water. The temperature of the extraction solvent can be appropriately set from room temperature to below the boiling point depending on the solvent used. In the present invention, ethanol or hydrous ethanol is preferable as the extraction solvent because the active ingredient can be efficiently extracted.

The content of ceramide is not particularly limited as long as it has a muscle-building effect and / or an anti-obesity effect, but is, for example, 0.000001 to 30%, preferably 0.00001 to the total amount of the composition. It is 20%, more preferably 0.0001 to 10%.

(Kuzunohana)
Kuzu is a climbing perennial plant of the genus Pueraria montana in the family Leguminosae. As the kudzu flower in the oral composition of the present invention, the one collected in any process from the bud to the fully opened flower may be used, or the one collected in each process may be mixed and used. The type of kudzu is not particularly limited, but Pueraria thomsonii, Pueraria lobata, Pueraria thunbergiana, etc. can be exemplified, and has a muscle-building effect and / or anti-virus. From the viewpoint of obesity effect, Pueraria thomsonii is preferable.

Examples of the kudzu flower in the oral composition of the present invention include processed products such as crushed products, juices, and extracts. Examples of the crushed product include powder, granules and the like, and for example, a crushed product after washing and drying can also be used. The juice or extract may be liquid, but it can also be used as a paste or a dry powder. The extract can be obtained by extracting with a suitable solvent, and the solvent may be, for example, water; lower alcohols such as ethanol, methanol, isopropanol and butanol; lower esters such as ethyl acetate and methyl acetate; acetone. ; Examples include a mixed solvent of these and water. The temperature of the extraction solvent can be appropriately set from room temperature to below the boiling point depending on the solvent used. In the present invention, the kudzu flower is preferably a pulverized product or an extract, more preferably an extract, and even more preferably a hot water extract from the viewpoint of muscle-building effect and / or anti-obesity effect.

The content of kudzu flower is not particularly limited as long as it has a muscle-building effect and / or an anti-obesity effect, but is, for example, 0.01 to 50% with respect to the total amount of the composition, preferably 0. It is 03 to 40%, more preferably 0.05 to 30%.

(Reynoutria sachalinensis)
Reynoutria sachalinense is a perennial plant belonging to the genus Ondate of the family Polygonum, and its scientific name is Polygonum sachalinense. Examples of the site to be used include leaves, stems, buds, roots, rhizomes and the like, and buds are particularly preferable. Buds are also called young shoots or sprouts. Examples of the Reynoutria sachalinensis in the oral composition of the present invention include treated products such as pulverized products, squeezed juices, and extracts. Examples of the crushed product include powder, granules and the like, and for example, a crushed product after washing and drying can also be used. The juice or extract may be liquid, but it can also be used as a paste or a dry powder. The extract can be obtained by extracting with a suitable solvent, and the solvent may be, for example, water; lower alcohols such as ethanol, methanol, isopropanol and butanol; lower esters such as ethyl acetate and methyl acetate; acetone. ; Examples include a mixed solvent of these and water. The temperature of the extraction solvent can be appropriately set from room temperature to below the boiling point depending on the solvent used. In the present invention, the Reynoutria sachalinensis is preferably a pulverized product or an extract, more preferably an extract containing a particularly large amount of an active ingredient, and even more preferably a hot water extract from the viewpoint of muscle-building effect and / or anti-obesity effect.

The content of Reynoutria sachalinensis is not particularly limited as long as it has a muscle-building effect and / or an anti-obesity effect, but is, for example, 0.0001 to 30%, preferably 0.001 to 0.001 to the total amount of the composition. It is 20%, more preferably 0.01 to 10%.

(Kotsusaiho (bone crushing supplement))
Kotsusaiho uses the rhizome of the Aglaomorpha fortunei (Drynaria fortunei) of the fern plant Fernaceae (Polypodiacea). In China, it is used as a Chinese herbal medicine to improve pain in bones and joints. Examples of the tips in the oral composition of the present invention include treated products such as pulverized products, juices, and extracts. Examples of the crushed product include powder, granules and the like, and for example, a crushed product after washing and drying can also be used. The juice or extract may be liquid, but it can also be used as a paste or a dry powder. The extract can be obtained by extracting with a suitable solvent, and the solvent may be, for example, water; lower alcohols such as ethanol, methanol, isopropanol and butanol; lower esters such as ethyl acetate and methyl acetate; acetone. ; Examples include a mixed solvent of these and water. The temperature of the extraction solvent can be appropriately set from room temperature to below the boiling point depending on the solvent used. In the present invention, Kotsusaiho is preferably a pulverized product or an extract, more preferably an extract containing a particularly large amount of an active ingredient, and further preferably ethanol or a hydrous ethanol extract from the viewpoint of muscle-building effect and / or anti-obesity effect. preferable.

The content of Kotsusaiho is not particularly limited as long as it has a muscle-building effect and / or an anti-obesity effect, but is, for example, 0.0001 to 30%, preferably 0.001 to 0.001 to the total amount of the composition. It is 20%, more preferably 0.01 to 10%.

(Muscle bone grass)
The musculoskeletal plant is a perennial plant belonging to the genus Bugleweed of the Labiatae family, and specific examples thereof include Ajuga decumbens, Ajuga ciliata, and Ajuga lupulina. Examples of the musculoskeletal grass in the oral composition of the present invention include treated products such as crushed products, juices, and extracts. Examples of the crushed product include powder, granules and the like, and for example, a crushed product after washing and drying can also be used. The juice or extract may be liquid, but it can also be used as a paste or a dry powder. The extract can be obtained by extracting with a suitable solvent, and the solvent may be, for example, water; lower alcohols such as ethanol, methanol, isopropanol and butanol; lower esters such as ethyl acetate and methyl acetate; acetone. ; Examples include a mixed solvent of these and water. The temperature of the extraction solvent can be appropriately set from room temperature to below the boiling point depending on the solvent used. In the present invention, the muscular bone grass is preferably a pulverized product or an extract, more preferably an extract containing a particularly large amount of an active ingredient, and even more so, ethanol and a hydrous ethanol extract from the viewpoint of muscle-building effect and / or anti-obesity effect. Is preferable.

The content of muscular bone grass is not particularly limited as long as it has a muscle-building effect and / or an anti-obesity effect, but is, for example, 0.0001 to 30%, preferably 0.001, based on the total amount of the composition. It is -20%, more preferably 0.01-10%.

(Capsicum)
The capsicum in the oral composition of the present invention is not particularly limited as long as it contains a capsaicin or a capsaicinoid-like substance. The variety and production area of capsicum are not particularly limited. Specifically, the capsicum varieties CH-19 sweet, Fushimi sweet pepper, shishito, Yamashina, Manganji, hawk's claw, Kagawamoto hawk, Aomori hawk's claw, Sapporo Daicho, California Wonder, Cherry Bomb, etc. can be used. can. Among them, Fushimi Kancho is preferably used because it contains both capsaicin and a capsaicinoid-like substance and has a low pungency. Various capsicums may be used alone or in combination of two or more.

As the capsicum in the oral composition of the present invention, any site may be used as long as it contains a capsaicin or a capsaicinoid-like substance. It is preferable to use fruits containing a sitting or placental part. In addition, the capsicum may be used raw or dried. For example, it can be used as a processed product such as a crushed product, squeezed juice, or an extract. Examples of the crushed product include powder, granules and the like. The juice or extract may be liquid, but it can also be used as a paste or a dry powder. The extract can be obtained by extracting with a suitable solvent, and the solvent may be, for example, water; lower alcohols such as ethanol, methanol, isopropanol and butanol; lower esters such as ethyl acetate and methyl acetate; acetone. ; Examples include a mixed solvent of these and water. The temperature of the extraction solvent can be appropriately set from room temperature to below the boiling point depending on the solvent used.

Further, the capsicum in the oral composition of the present invention may be fermented. The fermentation process decomposes, for example, capsicinoid-like substances contained in capsicum. The fermentation treatment is carried out by contacting with a microorganism capable of producing an organic acid and assimilating a fatty acid produced by decomposition of a capsaicinoid-like substance or the like. Capsaicinoid-like substances are decomposed by changes in pH due to organic acids produced by microorganisms.

Examples of fermentation include lactic acid fermentation, citric acid fermentation, alcoholic fermentation, acetic acid fermentation, and fermentation by a combination thereof. Depending on the type of fermentation, lactic acid bacteria, yeast, acetic acid bacteria, etc. are brought into contact with red pepper. These bacteria may be used alone for fermentation, a plurality of bacteria may be added at the same time and used for fermentation, or different bacteria may be added stepwise and used for fermentation. Among these, lactic acid fermentation is preferable.

Examples of lactic acid bacteria include Leuconostoc Mecentroides, Lactobacillus plantarum, Lactobacillus brevis, Lactobacillus acidophilus, Lactobacillus casei, Streptococcus thermophilus, Streptococcus faecalis, and Bifidobacterium longum. And used alone or in combination. For example, when used alone, Lactobacillus plantarum is suitable in terms of its acid resistance, growth temperature, and growth rate.

The content of capsicum is not particularly limited as long as it has a muscle-building effect and / or an anti-obesity effect, but is, for example, 0.0001 to 30%, preferably 0.001 to 0.001 to the total amount of the composition. It is 20%, more preferably 0.01 to 10%.

The oral composition of the present invention may be, for example, a pharmaceutical product (including a non-medicinal product), a food product for specified health use, a food product with nutritional function, a food product with a functional claim, or the like, a functional food product whose efficacy has been approved by a predetermined organization. It can be used as a so-called health food, general food, food additive, feed and the like.

The oral composition of the present invention can be used as an anti-obesity composition used for anti-obesity. The composition for anti-obesity is particularly limited as long as it contains HMB or a salt thereof and other materials and can be distinguished from other products as a product in that it is used for anti-obesity (suppression of obesity). For example, the body, packaging, instructions, or advertisement of the product according to the present invention has an anti-obesity function (including diet, reduction of body fat, improvement of metabolic syndrome, slimming, etc.). Is included in the scope of the present invention. The anti-obesity composition of the present invention is not limited to the one in which the component of the combination in the present invention (HMB or a salt thereof and other materials) is displayed as an active ingredient of anti-obesity on the packaging of the product or the like. For example, the active ingredient may not be specified, only HMB or a salt thereof may be labeled as the active ingredient, or only other materials may be labeled as the active ingredient.

Specific examples of the anti-obesity composition of the present invention include pharmaceuticals (including non-medicinal products) and so-called health foods. In so-called health foods, "for those who are concerned about body weight" and " "For those who are overweight", "For those who are concerned about body weight (BMI)", "Reduce weight and abdominal fat (visceral fat and subcutaneous fat)", "Reduce waist circumference", etc. It can be exemplified.

In addition, the oral composition of the present invention containing HMB or a salt thereof and other materials can be used as a muscle-building composition used for muscle-building. In particular, it is preferable to contain at least one selected from ceramide and kudzu flower together with HMB or a salt thereof. The composition for muscle building is particularly limited as long as it contains HMB or a salt thereof and other materials and can be distinguished from other products as a product in that it is used for muscle building and recovery from muscle fatigue. For example, muscle strengthening, enhancement of muscle synthesis, suppression of muscle decomposition, muscle mass (muscle weight, muscle cross-sectional area, muscle) in any of the main body, packaging, instruction manual, and advertisement of the product according to the present invention. Suppression / maintenance / increase of density), suppression / maintenance / improvement of muscle quality, suppression / maintenance / increase of muscle strength (power, endurance), suppression / maintenance / improvement of athletic performance, metabolism (basic metabolism) , Suppression / maintenance / improvement of metabolism during rest and exercise), Suppression / maintenance / increase of lean body mass, prevention / improvement of muscle fatigue, metabolism improvement effect by muscle strengthening, prevention / improvement effect of locomotive syndrome, sarcopenia The scope of the present invention includes those indicating that they have the function of preventing / improving the disease. The muscle-building composition of the present invention is not limited to the one in which the component of the combination in the present invention (HMB or a salt thereof and other materials) is displayed as an active ingredient for muscle-building on the packaging of the product or the like. For example, the active ingredient may not be specified, only HMB or a salt thereof may be labeled as an active ingredient, or only other materials may be labeled as an active ingredient.

Specific examples of the muscle-building composition of the present invention include pharmaceuticals (including non-medicinal products) and so-called health foods. In so-called health foods, "supporting the ability to build muscle" and "muscle" "Suppress the decomposition of muscles", "Strengthen muscle strength", "Suppress / maintain / improve / improve walking ability", "Improve metabolism by strengthening muscles", "Suppress the decline of metabolism", "Prevent muscle fatigue"・ Recovery ”,“ Suppression / maintenance of loss of balance ability ”,“ Shape up ”,“ Macho ”,“ Fine macho ”,“ Beautiful body ”,“ Prevention of sleeplessness ”,“ Prevention of sleeplessness ”,“ Prevention of falls ”,“ Muscle Examples of those displaying "improvement of metabolism by enhancement", "maintaining muscle mass and strength", etc. can be exemplified. The target for ingesting the oral composition of the present invention is not particularly limited as long as it is a person who needs muscle strengthening, but a person for the purpose of shape-up, an athlete, an elderly person with weak legs, etc. It can be preferably exemplified.

The anti-obesity effect and muscle-building effect of the oral composition of the present invention can be obtained by ingesting the composition of the present invention in daily life, but when used in combination with exercise, a more excellent effect can be obtained. Obtainable. The exercise referred to here is one or more of aerobic exercise and resistance exercise (strength training, weight training). In particular, when the muscle-building effect of the oral composition of the present invention is obtained, the type of exercise used in combination with the oral composition of the present invention is not particularly limited, but one or more of aerobic exercise and resistance exercise is carried out. It is preferable, and it is particularly preferable to carry out a resistance exercise. The amount of exercise when exercising is 10 minutes or more, preferably 20 minutes or more, and more preferably 30 minutes or more per day.

The form of the composition of the present invention includes, for example, tablets, capsules, powders, granules, liquids, granules, sticks, plates, blocks, solids, pills, pastes, creams, and caplets. Agents, gel agents, chewable tablets, stick agents and the like can be mentioned. Among these, tablets, capsules, powders, granules, pills and chewable tablets are preferable, and tablets, capsules, pills and chewable tablets are more preferable.

When the composition of the present invention is a tablet, a pill, or a chewable tablet, the tablet or pill obtained by adding one or more of an excipient, a lubricant, and a fluidizing agent while improving moldability is achieved. It is preferable because it improves the storage stability of the agent or chewable tablet. In particular, storage stability can be further enhanced by using excipients and lubricants. Excipients are added to improve the handling or molding of the composition and to make it more convenient to take. The excipient that can be used in the present invention is not particularly limited, and is, for example, starch, pregelatinized starch, partially pregelatinized starch, starch such as starch decomposition products or derivatives thereof, crystalline cellulose, powdered cellulose, sugar alcohol, lactose, beer. Examples thereof include yeast, low substitution hydroxypropyl cellulose, hydroxypropyl cellulose, purified sucrose, light anhydrous silicic acid, calcium silicate, titanium oxide, precipitated calcium carbonate, reduced maltose, maltose and the like. These may be used alone or in combination of two or more. In the present invention, hydroxypropyl cellulose, powdered cellulose, pregelatinized starch, pregelatinized starch, sugar alcohol, reduced maltose, and maltose are preferably used as excipients from the viewpoint of moldability and storage stability. The lubricant is used to alleviate the friction between the tableting machine and the tablet when compressing the powder for tablets, and to prevent tableting disorders such as sticking. The lubricant that can be used in the present invention is not particularly limited as long as it is a component that can achieve the above object, and for example, stearic acid such as stearic acid, calcium stearate, magnesium stearate or a salt thereof, fumaric acid. Examples thereof include stearyl sodium, sucrose fatty acid ester, talc, polyethylene glycol, vegetable oil and fat, and hydrogenated oil. These may be used alone or in combination of two or more. In the present invention, calcium stearate and sucrose fatty acid ester are preferably used as the lubricant from the viewpoint of moldability and storage stability. The fluidizing agent is used to improve the fluidity of mixed powders and granules. The fluidizing agent that can be used in the present invention is not particularly limited, and examples thereof include silicon dioxide, aluminum silicate, magnesium silicate aluminumate, calcium phosphate, magnesium carbonate, and magnesium oxide. These may be used alone or in combination of two or more. In the present invention, silicon dioxide and magnesium carbonate are preferably used as the fluidizing agent from the viewpoint of moldability and storage stability. In the present invention, commercially available products can be used as the excipient, the lubricant, and the fluidizing agent.

The content of HMB or a salt thereof and other materials (components of the present invention) in the composition of the present invention may be appropriately contained within the range in which the effect is exhibited.

Specifically, when the oral composition of the present invention is a supplement or pharmaceutical product of tablets, pills, capsule tablets, the component of the present invention may be contained in an amount of 5 to 99% by mass in terms of dry mass. It is more preferably contained in an amount of 8 to 98% by mass, and particularly preferably contained in an amount of 10 to 97% by mass. When the oral composition of the present invention is a chewable tablet supplement or a pharmaceutical product, the component of the present invention is preferably contained in an amount of 0.1 to 70% by mass in terms of dry mass, preferably 0.5 to 70% by mass. It is more preferably contained in an amount of 60% by mass, and particularly preferably contained in an amount of 1 to 50% by mass. In the case of powdery or granular supplements or pharmaceuticals, the components of the present invention are preferably contained in an amount of 0.1 to 90% by mass, preferably 0.5 to 80% by mass in terms of dry mass. Is more preferable, and it is particularly preferable that it is contained in an amount of 1 to 70% by mass. In the case of liquid supplements and pharmaceuticals, the components of the present invention are preferably contained in an amount of 5 to 99% by mass, more preferably 8 to 98% by mass, and 10 to 97% by mass in terms of dry weight. % Is particularly preferable.

The intake amount of the oral composition of the present invention is not particularly limited, but from the viewpoint of exerting the effect of the present invention more remarkably, the HMB intake per day for an adult is 100 mg / day or more. It is preferable to take it so as to be 200 mg / day or more, and it is further more preferable to take it so as to be 300 mg / day or more. The upper limit is, for example, 10000 mg / day, preferably 8000 mg / day, and more preferably 5000 mg / day. In addition, it is preferable that the daily intake of ceramide, kudzu flower, reynoutria sachalinensis, kotsusaiho, musculoskeletal grass, and capsicum is 0.1 mg / day or more, and 0.3 mg / day or more. It is more preferable to take it so as to be 0.5 mg / day or more. The upper limit is, for example, 1000 mg / day, preferably 500 mg / day, and more preferably 300 mg / day. The oral composition of the present invention may be appropriately designed so that the daily intake is the above-mentioned intake amount, and may be ingested once or in a plurality of times. For example, in the case of tablets, capsules, pills or chewable tablets, the number of ingestions is 1 to 4 times a day, and the total amount may be taken. The oral composition of the present invention can be contained in one container or divided into a plurality of containers, for example, 2 to 3 so that the daily intake becomes the above-mentioned intake, and can be contained as one day's worth.

The compounding mass ratio of HMB or a salt thereof and other materials is preferably in the range of 0.5: 1 to 100,000: 1, and preferably in the range of 0.75: 1 to 50,000: 1 in terms of dry mass. It is more preferably in the range of 1: 1 to 30000: 1, and particularly preferably in the range of 1: 1 to 10000: 1 from the viewpoint of muscle-building effect and / or anti-obesity effect.

The composition of the present invention can be produced by a known method by adding components other than the components of the present invention, if necessary. Examples of other components other than the components of the present invention include water-soluble vitamins (vitamins B1, B2, B3, B5, B6, B12, B13, B15, B17, biotin, choline, folic acid, inositol, PABA, vitamin C, etc. Vitamins such as vitamin P) and oil-soluble vitamins (vitamins A, D, E, K); minerals such as calcium, magnesium, phosphorus and iron; sulfur-containing compounds contained in taurine, garlic and the like; hesperidin, kelcetin and the like Flavonoids or flavonoids; proteins such as collagen; peptides; amino acids; animal fats and oils; vegetable fats and oils; crushed products or extracts of animals and plants.

Hereinafter, the present invention will be described based on examples.
[Example 1]
Test 1: Evaluation of adipose differentiation inhibitory effect using fibroblasts

(1) Cell culture (method for inducing differentiation into adipocytes)
Mouse fibroblast line (3T3-L1) was cultured in DMEM containing 10% (V / V) FBS in a 5% CO ₂ incubator at 37 ° C. using a 75 cm ² flask. Cells suspended by trypsin treatment were seeded from a 75 cm ² flask into each well of a collagen-coated 96-well plate at a cell density of 2 × 10 ⁴ cells / well. Incubate in a 5% CO ₂ incubator at 37 ° C until confluent. Three days after becoming confluent, a sample containing a test substance prepared in a differentiation-inducing medium was added and cultured for 7 days. At this time, the sample was replaced with a sample containing a test substance prepared in a differentiation maintenance medium every 2 to 3 days. Undifferentiated samples were cultured in DMEM containing 10% (V / V) FBS having the same concentration of dimethyl sulfoxide in the test substance-containing sample.

The differentiation-inducing medium was DMEM containing 10% (V / V) FBS, 0.5 mM of 3-isobutyl-1-methylxanthine (3-isobutyl-1-methylxanthine), and 0.5 μM of dexamethasone. Insulin prepared to be 10 μg / mL was used. In addition, the differentiation maintenance medium used was prepared so that the human insulin solution human was 10 μg / mL in DMEM containing 10% (V / V) FBS.

In addition, the following substances were used as test substances.
A commercially available product of HMBCa was used as HMB or a salt thereof.
As the ceramide, a purified product (commercially available) of rice-derived glucosylceramide having a sugar ceramide concentration of 99% or more was used.
As the kudzu flower, hot water extract powder of kudzu flower (manufactured by Toyo Shinyaku Co., Ltd.) was used.
Hot water extract powder (commercially available) of Reynoutria sachalinensis was used as Reynoutria sachalinensis.
As Kotsusaiho, ethanol extract powder (commercially available) of Kotsusaiho was used.
As the muscle bone grass, ethanol extract powder (commercially available product) of muscle bone grass was used.
As the capsicum, "Ao capsicum fermented extract" (manufactured by Toyo Shinyaku Co., Ltd.), which is a fermented extract of lactic acid bacteria of Fushimi Kancho, was used.

(2) Staining of intracellular lipid droplets To the cells after culturing, an equal amount of 10% formalin solution was added to 100 μL of the sample, and the cells were allowed to stand at room temperature for 10 minutes in the dark. The formalin solution was removed, a new 10% formalin solution was added to the cells at 100 μL / well, and the cells were allowed to stand at room temperature for 10 minutes in the dark, and the cells were fixed. The formalin solution was removed and washed twice with PBS. A 60% isopropanol-oil red solution was added to the cells and blank wells at 50 μL / well and allowed to stand at room temperature for 30 minutes in the dark to stain the lipid droplets. The stain was removed and 60% isopropanol was added at 150 μL / well. 60% isopropanol was removed and washed once with PBS. 50 μL / well of 100% isopropanol was added to the cells and the blank well, and the mixture was shaken for about 10 minutes to extract the stain. The absorbance of the isopropanol solution from which the staining solution was extracted was measured at 520 and 650 nm (turbidity).
(3) Protein quantification method The isopropanol solution was allowed to stand at room temperature for 1 day to completely remove the isopropanol in the plate. After removing the isopropanol, 20 μL / well of PBS was placed in a 96-well plate and allowed to stand in a freezer at −80 ° C. until it was completely frozen. The 96-well plate was removed from the -80 ° C freezer and allowed to stand at room temperature until completely thawed. The reaction solution of the protein assay BCA kit was added at 160 μL / well. As Standard, BSA final concentrations of 0,25,125,250,500,750,1000,2000 μg / mL were prepared. After gently shaking with a plate shaker, the mixture was incubated at 37 ° C. for 30 minutes. After incubation, the supernatant returned to room temperature was collected at 120 μL / well and transferred to another 96-well plate. The absorbance at 562 nm was measured.
(4) Data analysis Based on the obtained data, "% of control" was calculated from the following formula.

% Of control =
[Data520nm-Data650nm] / [Protein concentration] x 100

In the formula, the protein concentration was calculated by drawing a calibration curve (y = Ax + B) from the absorbance of Standard. Further, Data 520 nm is a value of absorbance at 520 nm after oil red staining, Data 650 nm is a value of absorbance at 650 nm (turbidity) after oil red staining, and Control is [Value of Data 562 nm]-[Standard 0]. Is the value of.

FIGS. 1 to 6 show the evaluation results of the fat mass of mouse fibroblasts. The numerical value indicates that the lower the value, the more the differentiation of adipocytes was suppressed. From the left, each figure shows the results of "control", "single addition of HMBCa", "single addition of other materials", and "addition of HMBCa + other materials", and the concentration unit of the added component is μg / mL. be.

As shown in FIGS. 1 to 6, the composition of the present invention using HMBCa and other materials of the present invention synergistically suppressed the differentiation of adipocytes as compared with the case of each material alone. Since obesity is due to hypertrophy and proliferation of adipocytes, it is considered that obesity can be prevented by suppressing the differentiation of adipocytes. Therefore, the oral composition of the present invention is useful for obesity prevention.

Test 2: Evaluation of muscle differentiation promoting action using myoblasts (1) 10% (V /) of mouse myoblast line (C2C12) in a 75 cm ² flask in a 5% CO ₂ incubator at 37 ° C. V) Cultured in DMEM containing FBS.
(2) Cells suspended by trypsin treatment were seeded from a 75 cm ² -flask to each well of a 96-well plate at a cell density of 5000 cells / well.
(3) The cells were pre-cultured at 37 ° C. in a 5% CO ₂ incubator for 72 hours.

(4) 200 μL of the test substance-containing medium adjusted to a predetermined concentration in DMEM containing 0.5% (V / V) DMSO-10% (V / V) FBS was added, and the cells were cultured for 24 hours.
(5) After culturing for 24 hours, RNA was recovered using RNeasy Mini Kit (manufactured by QIAGEN), and cDNA was synthesized using RiverTra Ace (registered trademark) qPCR RT Master Mix with gDNA Remember (manufactured by Toyobo).
(6) Using the obtained cDNA as a template, quantitative real-time PCR was performed by QuantiNova SYBR Green PCR Kit (manufactured by QIAGEN) using a primer (manufactured by QIAGEN) for the Myogenin gene (Myog), and the mRNA expression level of the Myogenin gene was measured. did. As an endogenous control, the mRNA expression level of GAPDH was measured using a GAPDH primer (manufactured by QIAGEN).

The following substances were used as test substances.
A commercially available product of HMBCa was used as HMB or a salt thereof.
As the ceramide, a purified product (commercially available) of rice-derived glucoside ceramide having a sugar ceramide concentration of 99% or more was used.
As the kudzu flower, hot water extract powder of kudzu flower (manufactured by Toyo Shinyaku Co., Ltd.) was used.

7 and 8 show the measurement results of the mRNA expression level of the Myogenin gene. The Myogenin gene is a gene that acts when myoblasts differentiate into muscle cells, and the mRNA expression level of the Myogenin gene is an index of muscle cell differentiation. The higher the value, the higher the mRNA expression level of the Myogenin gene. From the left, each figure shows the results of "control", "single addition of HMBCa", "single addition of other materials", and "addition of HMBCa + other materials", and the concentration unit of the added component is μg / mL. be.

As shown in FIGS. 7 and 8, the composition of the present invention using HMBCa and a specific material showed a synergistically higher mRNA expression level of the Myogenin gene as compared with the case of each material alone. From these results, it is considered that the composition of the present invention can effectively promote the differentiation of myoblasts into muscle cells in skeletal muscle and more effectively enhance skeletal muscle.

[Example 2] (Manufacturing of tablets)
A tablet (250 mg) consisting of the following components was produced. Ingest 5 tablets per day.

HMBCa 50%
Kuzunohana hot water extract 25%
Calcium stearate 2%
Silicon dioxide 2%
Reduced maltose 21%

[Example 3] (Manufacturing of tablets)
A tablet (350 mg) consisting of the following components was produced. Ingest 6 tablets per day.

HMBCa 85%
Rice-derived glucosylceramide 0.1%
Pullulan 1%
Reduced maltose 13.9%

When the above tablets are taken with water once or divided into two or three times a day, excellent muscle-building effect and anti-obesity effect can be obtained.

[Example 4] (Production of capsule)
The following mixture was encapsulated in a hard capsule to produce a capsule (300 mg). Ingest 5 of the obtained hard capsules per day.

HMBCa 70%
Reynoutria sachalinensis hydrous ethanol extract 0.5%
Kotsusaiho Hydrous Ethanol Extract 0.5%
Muscle bone grass hot water extract 0.5%
Capsicum ethanol extract 0.5%
Lactic acid bacteria 5%
Cellulose 21%
Silicon dioxide 2%

When the capsule is taken once a day or divided into 2 to 4 times with water, an excellent muscle-building effect and an anti-obesity effect can be obtained.

[Example 5] (Production of granules)
The following components were mixed to prepare granules (3000 mg) by a conventional method. By taking the obtained granules together with water, excellent muscle-building effect and anti-obesity effect can be obtained.

HMBCa 50%
Kuzunohana water extract 10%
Corn-derived glucosylceramide 2%
Aspartame 0.1%
Thiamine hydrochloride 0.33%
Riboflavin 0.33%
Vitamin B6 0.17%
Cyanocobalamin 0.17%
Fragrance 0.17%
Reduced palatinose 6.67%
Calcium stearate 3.33%
Hirodoxypropyl Cellulose Remaining

[Example 6] (Manufacturing of chewable tablets)
A chewable tablet (1000 mg per tablet) consisting of the following components was produced. By ingesting the obtained chewable tablets 3 times a day, 2 tablets (6 tablets in total), excellent muscle-building effect and anti-obesity effect can be obtained.

HMBCa 20.00%
Kuzunohana hot water extract 15.00%
Kotsusaiho Water Extract 0.70%
Muscle bone grass ethanol extract 0.70%
Sucralose 0.10%
Aspartame 0.05%
Vitamin B1 0.01%
Vitamin B2 0.01%
Vitamin B6 0.01%
Fragrance 0.01%
Calcium Stearate 1.00%
Silicon dioxide 2.00%
Hydroxypropyl cellulose 1.00%
Cellulose 30.00%
Reduced palatinose balance

[Example 7] (Manufacturing of chewable tablets)
A chewable tablet (700 mg per tablet) consisting of the following ingredients was produced. By ingesting two of the obtained chewable tablets per day, excellent muscle-building effect and anti-obesity effect can be obtained.

HMBCa 40.00%
Reynoutria sachalinensis hydrous ethanol extract 0.70%
Kotsusaiho Ethanol Extract 0.70%
Muscle bone grass hot water extract 0.70%
Fragrance 0.01%
Sucrose fatty acid ester 3.00%
Silicon dioxide 2.00%
Hydroxypropyl cellulose 5.00%
Reduced palatinose balance

Since the oral composition of the present invention has a muscle-building effect, an anti-obesity effect and the like, the industrial usefulness of the present invention is high.

Claims (6)

An oral composition containing 3-hydroxy-3-methylbutyric acid or a salt thereof as an active ingredient of anti-obesity, which further contains ceramide. An oral composition containing 3-hydroxy-3-methylbutyric acid or a salt thereof as an active ingredient for muscle building, and further containing ceramide (excluding black rice) for human muscles. Oral composition for enhancement. An anti-obesity oral composition containing 3-hydroxy-3-methylbutyric acid or a salt thereof and ceramide .
An oral composition for anti-obesity, wherein the 3-hydroxy-3-methylbutyric acid or a salt thereof is an active ingredient having a function of helping to reduce body fat. An oral composition for maintaining muscle strength containing 3-hydroxy-3-methylbutyric acid or a salt thereof and ceramide (excluding black rice) .
It is characterized that 3-hydroxy-3-methylbutyric acid or a salt thereof is an active ingredient of a function useful for maintaining / suppressing a decrease in muscle strength necessary for living an independent daily life and / or maintaining / improving walking ability. Oral composition for maintaining muscle strength for humans. An oral composition for anti-obesity, which comprises 3-hydroxy-3-methylbutyric acid or a salt thereof and ceramide. An oral composition for muscle building for humans, which comprises 3-hydroxy-3-methylbutyric acid or a salt thereof and ceramide (excluding black rice) .

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