JP2019043863A - UCP expression promoter - Google Patents

Abstract

To provide an agent and a food and drink showing a UCP expression promoting action.SOLUTION: A UCP expression promoter contains one or plural compounds selected from the group consisting of a lophenol compound and a cyclolanostan compound as an active ingredient.SELECTED DRAWING: None

Description

  The present invention relates to a UCP expression promoter.

  Uncoupling protein (hereinafter referred to as UCP) is known as a thermogenic molecule which uncouples oxidative phosphorylation in mitochondria and dissipates oxidation energy as heat. Here, UCP1 is widely distributed in brown adipose tissue, UCP2 is widely distributed in white adipose tissue, skeletal muscle, spleen, small intestine, etc., and UCP3 is mainly expressed in skeletal muscle (patent documents 1, 2, non-patent, Documents 1 and 2).

  UCP2 has been reported to have actions such as amelioration of nervous system damage, promotion of nervous system development, or prevention of decline in brain function (Non-patent Document 3).

  UCP1 and UCP3 are also known to be associated with muscle wasting diseases such as sarcopenia. (Non-patent documents 4, 5 and 6)

As a prior art, it is known that a black moth (Kaempferia parviflora) enhances the expression of UCP1 (patent document 3).
In addition, it is known that resveratrol enhances the expression of UCP2 (Patent Document 4).
Moreover, the extract of epigallocatechin and mugwort is mentioned as a raw material which has the effect | action which enhances the expression of UCP3 (patent documents 5 and 6).

  By the way, for a compound having a cyclolanostane skeleton or a compound having a rophenol skeleton, utilization for preventing or ameliorating a symptom caused by disturbance in the balance of a sex hormone has been proposed (Patent Document 7).

Japanese Patent Application Publication No. 2013-515488 JP-A-2017-507670 JP 2017-88616 A JP, 2010-24208, A JP, 2013-177334, A JP, 2013-216606, A International Publication No. 2016/0894956 Pamphlet

Japanese pharmacology journal 118 (5), 2001, p327-333. Proceedings of the 124th Japan Medical Association Symposium p62-70. Cellular Signaling, 2008, April: Volume 20, Issue 4, Pages 645-658. Shikoku Medical Journal, 2014, DECEMBER 25, 70, 5, 6, 149-154. Sports Health Science Research 2013 35: 1-16. "Sarcopenia: Consensus and Q & A of European Associations on Definition and Diagnosis", [pdf], Health and Labor Science Research Grant (Longevity Science Research Project) Preventive measures for age-related muscle weakness (sarcopenia) in elderly people Comprehensive research for establishing research research group, [July 13, 2017 search], Internet <URL: http://www.jpn-geriat-soc.or.jp/info/topics/pdf/sarcopenia_EWGSOP_jpn-j -geriat2012.pdf>

As described in Patent Documents 3 to 6, while materials showing a UCP expression promoting action have been proposed, development of materials that can be safely consumed has been further demanded.
An object of the present invention is to provide a drug and a food and drink that can be taken safely safely on a daily basis and show UCP expression promoting action without causing pain as much as possible.

  The present inventors have found that one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds have a UCP expression promoting action, and completed the present invention.

  That is, the present invention for solving the above problems is a UCP expression promoter comprising, as an active ingredient, one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds.

  In a preferred embodiment of the present invention, one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds are 4-methylcholest-7-en-3-ol, 4-methylergost-7- Consisting of ene-3-ol, 4-methylstigmast-7-en-3-ol, 9,19-cyclolanostan-3-ol, 24-methylene-9,19-cyclolanostan-3-ol It is one or more compounds selected from the group.

  Moreover, as for this invention, it is more preferable to set it as the form which contains the said compound in total amount 0.00001 mass% or more.

  The present invention is also a UCP expression promoter comprising, as an active ingredient, a composition containing 0.00001% by mass or more of one or more compounds selected from the group consisting of rophenol compounds and cyclolanostane compounds.

  Furthermore, in the UCP expression promoter of the present invention, it is preferable that the expression promotion target is UCP2.

  The UCP expression promoter of the present invention whose expression promotion target is UCP2 is preferably in a form used for amelioration of nervous system damage, promotion of nervous system development, and / or prevention of a decrease in brain function.

  Further, in the UCP expression promoter of the present invention, it is preferable that the expression promotion target is UCP1 and / or UCP3.

  The UCP expression promoter of the present invention whose expression promotion target is UCP1 and / or UCP3 is preferably in a form used for the prevention and / or improvement of sarcopenia.

  In addition, the present invention is also present in a food and drink composition for promoting UCP expression, which comprises, as an active ingredient, one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds.

  In a preferred embodiment of the food and drink composition for promoting UCP expression according to the present invention, one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds are 4-methylcholest-7-en-3-ol 4-Methylergost-7-en-3-ol 4-Methylstigmust-7-en-3-ol 9,19-Cyclolanostan-3-ol 24-Methylene-9,19- It is one or more compounds selected from the group consisting of cyclolanostan 3-ol.

  Further, the food and drink composition for promoting UCP expression of the present invention more preferably contains the above-mentioned compounds in a total amount of 0.00001% by mass or more.

  In addition, the present invention relates to a food and drink composition for promoting UCP expression, comprising, as an active ingredient, a composition containing 0.00001% by mass or more of one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds. It is also a thing.

  Moreover, as for the food-drinks composition for UCP expression promotion of this invention, it is preferable that expression promotion object is UCP2.

  The food composition for promoting UCP expression of the present invention, whose expression promoting target is UCP2, is a form used for ameliorating nervous system damage, promoting nervous system development and / or preventing brain function decline. Is preferred.

  Further, in the food and drink composition for promoting UCP expression of the present invention, it is preferable that the expression promotion target is UCP1 and / or UCP3.

  The food / drink composition for promoting UCP expression of the present invention whose expression promoting target is UCP1 and / or UCP3 is preferably in a form used for preventing and / or improving sarcopenia.

  Next, preferred embodiments of the present invention will be described in detail. However, the present invention is not limited to the following preferred embodiments, and can be freely modified within the scope of the present invention. In the present specification, percentages are indicated by mass unless otherwise specified.

  The UCP expression promoter of the present invention contains, as an active ingredient, a compound selected from the group consisting of a lophenol compound (compound 1) and a cyclolanostane compound (compound 2). The compound 1 and the compound 2 are represented by the following general formula (1) and general formula (2), respectively.

In general formula (1), R1 is a linear or branched alkyl group having 5 to 16 carbon atoms, or an alkenyl group containing one or two double bonds. In addition, the alkyl group or alkenyl group may be a substituted alkyl group or substituted alkenyl group in which one or two hydrogen atoms are substituted with a hydroxyl group and / or a carbonyl group.
Moreover, R2 and R3 are respectively independently a hydrogen atom or a C1-C3 alkyl group. Here, as said C1-C3 alkyl group, a methyl group, an ethyl group, etc. are preferable, and a methyl group is especially preferable. In addition, the alkyl group may be a substituted alkyl group in which at least one hydrogen atom is substituted with a hydroxyl group and / or a carbonyl group.

  In addition, R 4 forms C = O together with the carbon atom constituting the ring, or is —OH or —OCOCH 3.

  In the general formula (1), R 1 is preferably any one of the groups represented by the following formula.

  In the general formula (1), one of R2 and R3 is a hydrogen atom, the other is preferably a methyl group, and R4 is preferably a hydrogen group.

  Compound 1 preferably includes 4-methylcholest-7-en-3-ol, 4-methylergst-7-en-3-ol and 4-methylstigmast-7-en-3-ol. . Each compound has a structure represented by the following formula.

Compound 1 can be produced chemically according to known production methods.
For example, Vitali Matyash et al. , PLOS BIOLOGY, Volume 2, Issue 10, e280, 2004. According to the supplement data described, it is possible to synthesize.

Further, it is known that the compound 1 is contained in plants, and the compound 1 can be produced according to a known method for producing rophenol (Biochemical Experimental Method 24, Lipolipid Metabolism Experimental Method, Yamada Takahiro, Academic Press Center, page 174 (1989).
For example, it is possible to extract from a plant known to contain Compound 1 using a method such as a hot water extraction method, an organic solvent extraction method, a supercritical extraction method or a subcritical extraction method (for example, , 3905913)). The compound 1 can be extracted, for example, from plants of the liliaceae, leguminous family, gramineaceous family, solanaceous family and muskaceae family.
The compound 1 produced as described above can have its molecular weight, structure, etc. determined or confirmed by, for example, mass spectrum (MS) method, nuclear magnetic resonance spectrum (NMR) method or the like.

Compound 1 may also be a pharmaceutically acceptable salt. Pharmaceutically acceptable salts include both metal salts (inorganic salts) and organic salts, a list of which is given in "Remington's Pharmaceutical Sciences", 17th ed., 1985. What is listed in the year 1418 tribute is illustrated.
Specifically, inorganic acid salts such as hydrochloride, sulfate, phosphate, diphosphate and hydrobromide, malate, maleate, fumarate, tartrate, succinate Non-limiting examples include organic acid salts such as citrate, acetate, lactate, methanesulfonate, p-toluenesulfonate, pamoate, salicylate, and stearate.
In addition, salts of metals such as sodium, potassium, calcium, magnesium and aluminum, and salts with amino acids such as lysine can also be used. In addition, solvates such as hydrates of the compounds or pharmaceutically acceptable salts thereof can also be used.

In general formula (2), R 5 is a linear or branched alkyl group having 6 to 8 carbon atoms, or an alkenyl group containing one or two double bonds. In addition, the alkyl group or alkenyl group may be a substituted alkyl group or substituted alkenyl group in which one or two hydrogen atoms are substituted with a hydroxyl group and / or a carbonyl group.
R6 and R7 each independently represent a hydrogen atom or a methyl group. Further, R 8 forms CCO together with the carbon atom constituting the ring, or is any of the following formulas.

  In the general formula (2), R5 is preferably any one of the groups represented by the following formula.

  In the general formula (2), it is preferable that one of R 6 and R 7 is a hydrogen atom, and the other is a methyl group, and it is preferable that R 8 be a hydroxyl group.

  Compound 2 preferably includes 9,19-cyclolanostan-3-ol and 24-methylene-9,19-cyclolanostan-3-ol. Each compound has a structure represented by the following formula.

  Compound 2 can be produced chemically according to known production methods. For example, 24-methylene-9,19-cyclolanostan-3-ol (common name: 24-methylenecycloaltanol) is disclosed in JP-A-57-018617 and WO 2012/023599 (γ-oryzanol). Can be produced according to the method disclosed in Moreover, it is possible to manufacture the hydrolyzate of cycloartenol ferulate as a starting material by the method disclosed by Unexamined-Japanese-Patent No. 2003-277269.

Compound 2 is also known to be contained in plants such as liliaceae, legumes, grasses, solanaceous and muskaceae ([Phytochemistry, US, Volume 16 of 1977]. , Pages 140-141], [Handbook of Phytochemical Constituents of GRAS, Herbs and Other Economic Plants, Handbook of Phytochemical Constituents of GRAS herbs and other economic plants, 1992]. U.S.C., C. Shipress, or [Hagels-Huntbuch-Der-Farmazoi-ticsin-Plaxis] (Hager's Handbuch der Pharmazeutisc en Praxis), second to sixth Volume, 1969-1979 years, Germany, Springer-Verlag Berlin] reference). Therefore, compound 2 can be extracted from these plants using a known method such as an organic solvent extraction method or a hot water extraction method (see, for example, Japanese Patent No. 3924310). The compound 2 is preferably extracted from a plant of the genus Liliaceae Aloe.
The molecular weight, the structure, and the like of the compound produced as described above can be determined or confirmed by, for example, a mass spectrum (MS) method, a nuclear magnetic resonance spectrum (NMR) method, or the like.

  Compound 2 may also be a pharmaceutically acceptable salt. Such salts are as exemplified for Compound 1.

The UCP expression promoter of the present invention contains a compound selected from the group consisting of Compound 1 and Compound 2 as an active ingredient. The compound may be a single compound, that is, either Compound 1 or Compound 2 alone, or a mixture of Compound 1 and Compound 2.
When Compound 1 or Compound 2 is used alone, Compound 1 (mainly 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol, or 4-methyls) is used. Either tigmast-7-en-3-ol) or compound 2 (mainly 9,19-cyclolanostan-3-ol or 24-methylene-9,19-cyclolanostan-3-ol) Is preferred.
Among them, 4-methylcholest-7-en-3-ol is particularly preferable as Compound 1 in terms of physical properties such as solubility to be considered when used as an active ingredient of a UCP expression promoter, and 9 as Compound 2 19-Cyclolanostan-3-ol is particularly preferred.
In the case where Compound 1 and Compound 2 are compared, Compound 1 (mainly, 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol or 4-methylstig) More preferably, it is mast-7-en-3-ol).
In each of Compound 1 and Compound 2, one type of compound may be used, or a plurality of compounds may be mixed and used.
The UCP expression promoter of the present invention is preferably 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol, 4-methylstigmast-7-en-3 It contains as an active ingredient a compound selected from the group consisting of -ol, 9,19-cyclolanostan-3-ol and 24-methylene-9,19-cyclolanostan-3-ol.

In the case where both of the compound 1 and the compound 2 are combined (a mixture of the compound 1 and the compound 2), the range of the mass ratio of the compound 1 and the compound 2 is, for example, the following.
Compound 1: Compound 2 is preferably 5: 1 to 1: 5, more preferably 3: 1 to 1: 3, particularly preferably 2: 1 to 1: 2.

  The content of the compound in the UCP expression promoter of the present invention can be appropriately selected according to the symptoms and the like, but in total, preferably at least 0.00001% by mass, more preferably at least 0.0001% by mass. More preferably, it is at least 0.0005% by weight, particularly preferably at least 0.001% by weight. The upper limit of the amount in the UCP expression promoter of the present invention is not particularly limited, but a total amount of 90% by mass or less, preferably 70% by mass or less, more preferably 50% by mass or less is exemplified.

Moreover, the UCP expression promoter of this invention can also be made into the form which contains the composition which contains 0.00001 mass% or more of compounds selected from the group which consists of a compound 1 and a compound 2 as an active ingredient.
As such a composition, for example, an extract obtained from a plant containing Compound 1 described above, an extract obtained from a plant containing Compound 2 and a plant containing both Compound 1 and Compound 2 can be used. Extracts, as well as mixtures thereof.

  Here, as a plant containing the compound 1 and the compound 2, plants such as liliaceae, leguminous family, gramineous family, solanaceous family, and spinach family can be mentioned, for example.

  As an example included in natural plants, compound 1 (mainly 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol and 4- 4 Methylstigmast-7-en-3-ol), and compound 2 (mainly 9,19-cyclolanostan-3-ol and 24-methylene-9,19-cyclolanostan-3-ol) It is known to be included.

  Therefore, using aloe vera as a raw material, 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol, or 4-methylstigmast-7-en-3-ol Any one of (Compound 1) or any one of 9,19-cyclolanostan-3-ol or 24-methylene-9,19-cyclolanostan-3-ol (compound 2) is purified respectively, Compound 1: It is possible to obtain mixtures in which the compound 2 comprises 5: 1 to 1: 5, preferably 3: 1 to 1: 3, particularly preferably 2: 1 to 1: 2. The composition thus obtained is suitable as an active ingredient of the UCP expression promoter of the present invention.

  In addition, the UCP expression promoter of the present invention is a total of one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds, more preferably at least 0.0001% by mass, still more preferably at least It is preferable to use a composition containing 0.0005% by mass, particularly preferably at least 0.001% by mass, as an active ingredient.

The agent for promoting UCP expression of the present invention can be used in the form of a medicine or a pharmaceutical composition.
The agent for promoting UCP expression of the present invention can be orally or parenterally administered to mammals including human.

The agent for promoting UCP expression of the present invention has an activity for promoting expression of UCP2.
Here, UCP2 is one of the components of neurons that are particularly abundant in the brain, and it is known that UCP2 deficiency causes brain nervous system problems (Cellular Signaling, 2008, April: Volume 20, Issue) 4, Pages 645-658).

That is, by promoting the expression of UCP2, amelioration of nervous system damage, promotion of nervous system development, and / or prevention of reduction in brain function are exerted.
Therefore, the UCP expression promoter of the present invention can be used to ameliorate nervous system damage, promote nervous system development, and / or prevent brain function decline.

  As used herein, the term "prevention" includes the reduction of the risk of developing a disease. Also, the concept of "improvement" includes both treatment and alleviation of symptoms.

  Here, damage to the nervous system includes the central nervous system (brain, brainstem and cerebellum), the peripheral nervous system (including the cranial nerve) and the autonomic nervous system (part of which is in both the central nervous system and the peripheral nervous system). Includes diseases or disorders that affect. Then, diseases caused by damage to the nervous system include diseases such as headache, sleep drowsiness, dementia, seizures, sleep disorder, trauma, movement disorder, demyelinating disease, spinal cord disorder peripheral nerve, and the like.

  Here, the decrease in brain function includes a decrease in brain function caused by stress, a decrease in brain function caused by aging, and a decrease in brain function caused by a disease such as an accident or a stroke. And, by preventing the decline in brain function, for example, effects such as prevention of decline in memory ability, prevention of decline in interest of interest, prevention of moodiness (irritability) and the like can be obtained.

The agent for promoting UCP expression of the present invention has an activity for promoting the expression of UCP1 and UCP3.
Here, it is preferable that UCP expression promoter having UCP1 and UCP3 expression promoting action is a form used for the prevention and / or improvement of sarcopenia.
In addition to sarcopenia, UCP expression promoters for promoting UCP1 and UCP3 are, as sarcopenia, cancer, AIDS, sepsis, COPD, renal failure, arthritis, congestive heart failure, muscular dystrophy, and no It can also be used to prevent or improve the feeling of weight.

  The form of the UCP expression promoter of the present invention is not particularly limited, and can be appropriately selected according to the method of use. Specifically, tablets, pills, powders, solutions, suspensions, emulsions, granules, capsules, syrups, suppositories, injections, ointments, patches, eye drops, nasal drops etc. are exemplified. it can.

The administration time of the UCP expression promoter of the present invention is not particularly limited, and can be appropriately selected according to the target disease. In addition, it is preferable that the dose be determined according to the form of the preparation, dosage, age, sex of the patient, other conditions, degree of symptoms and the like.
The dose of the UCP expression promoter of the present invention is appropriately selected according to the method of use, the age, sex, degree of disease, other conditions, etc. of the patient. In general, the range of 0.0001 to 100 mg / day, more preferably 0.001 to 50 mg / day, and particularly preferably 0.01 to 10 mg / day is considered as a standard in terms of the amount of the active ingredient.

  The UCP expression promoter of the present invention may contain additives widely used in medicine. The additives include excipients, binders, disintegrants, lubricants, stabilizers, flavoring agents, diluents, surfactants, solvents for injections and the like.

The UCP expression promoter of the present invention can be produced by blending the compound as an active ingredient into a pharmaceutical carrier. The UCP expression promoter of the present invention can be produced, for example, by formulating the above-mentioned compound with the above-mentioned additive.
Further, the UCP expression promoter of the present invention is an extract obtained by extraction using supercritical water or subcritical extraction using hot water or various solvents, using a known plant or the like containing the compound as a raw material, It can also be manufactured by formulating with the added additives.
In particular, the UCP expression promoter of the present invention containing Compound 1 and Compound 2 in the range of the above-mentioned specific weight ratio can be produced by mixing each compound in the range of the above-mentioned weight ratio. Moreover, such a medicine is manufactured by methods, such as extraction using a hot water and various solvents, supercritical extraction, subcritical extraction, etc. by using as a raw material the well-known plant etc. in which the compound 1 and the compound 2 are contained. It is also possible.

  The UCP expression promoter of the present invention can be obtained, for example, from a plant such as liliaceae, leguminous family, gramineous family, solanaceous family, and spinach family.

  The UCP expression promoter of the present invention has the compound acting as an active ingredient, and has a preventive or ameliorating effect on symptoms caused by the decrease in UCP activity. In particular, it is effective for the prevention or amelioration of symptoms caused by the decrease in activity of any UCP selected from the group consisting of UCP1, UCP2 and UCP3.

  The present invention is also a food and drink composition for promoting UCP expression. In the present invention, the “food and drink composition” includes, in addition to the food and drink that humans consume, a feed that animals other than humans consume.

The food and drink composition for promoting UCP expression of the present invention contains a compound selected from the group consisting of Compound 1 and Compound 2 as an active ingredient. The compound may be a single compound, that is, either Compound 1 or Compound 2 alone, or a mixture of Compound 1 and Compound 2.
When Compound 1 or Compound 2 is used alone, Compound 1 (mainly 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol, or 4-methyls) is used. Either tigmast-7-en-3-ol) or compound 2 (mainly 9,19-cyclolanostan-3-ol or 24-methylene-9,19-cyclolanostan-3-ol) Is preferred.
Among them, 4-methyl cholest-7-en-3-ol is particularly preferable as compound 1 in terms of physical properties such as solubility considered when used as an active ingredient of a UCP expression promoting food and drink composition, compound 2 Particularly preferred is 9,19-cyclolanostan-3-ol.
In the case where Compound 1 and Compound 2 are compared, Compound 1 (mainly, 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol or 4-methylstig) More preferably, it is mast-7-en-3-ol).
In each of Compound 1 and Compound 2, one type of compound may be used, or a plurality of compounds may be mixed and used.
The food and drink composition for promoting UCP expression of the present invention is preferably 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol, 4-methylstigmast-7. It contains as an active ingredient a compound selected from the group consisting of -en-3-ol, 9,19-cyclolanostan-3-ol and 24-methylene-9,19-cyclolanostan-3-ol.

In the case where both of the compound 1 and the compound 2 are combined (a mixture of the compound 1 and the compound 2), the range of the mass ratio of the compound 1 and the compound 2 is, for example, the following.
Compound 1: Compound 2 is preferably 5: 1 to 1: 5, more preferably 3: 1 to 1: 3, particularly preferably 2: 1 to 1: 2.

  The content of the compound in the food and drink composition for promoting UCP expression of the present invention can be appropriately selected according to the symptoms and the like, but in total, preferably at least 0.00001% by mass, more preferably at least 0. It is 0001% by weight, more preferably at least 0.0005% by weight, particularly preferably at least 0.001% by weight. The upper limit of the amount in the food and drink composition for promoting UCP expression of the present invention is not particularly limited, but the total amount is 90% by mass or less, preferably 70% by mass or less, more preferably 50% by mass or less.

The food and drink composition for promoting UCP expression of the present invention contains, as an active ingredient, a composition containing 0.00001% by mass or more of a compound selected from the group consisting of Compound 1 and Compound 2. The compound may be used alone or in combination.
As such a composition, for example, an extract obtained from a plant containing Compound 1 described above, an extract obtained from a plant containing Compound 2 and a plant containing both Compound 1 and Compound 2 can be used. Extracts, as well as mixtures thereof.

  For example, as an example contained in natural plants, compound 1 (mainly 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol and 4-Methylstigmast-7-en-3-ol), and compound 2 (mainly 9,19-cyclolanostan-3-ol and 24-methylene-9,19-cyclolanostan-3-ol ) Is known to be included.

  Therefore, using aloe vera as a raw material, 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol, or 4-methylstigmast-7-en-3-ol Any one of (Compound 1) or any one of 9,19-cyclolanostan-3-ol or 24-methylene-9,19-cyclolanostan-3-ol (compound 2) is purified respectively, Compound 1: It is possible to obtain mixtures in which the compound 2 comprises 5: 1 to 1: 5, preferably 3: 1 to 1: 3, particularly preferably 2: 1 to 1: 2. The composition thus obtained is suitable as an active ingredient of the food and drink composition for promoting UCP expression of the present invention.

  In addition, the food and drink composition for promoting UCP expression of the present invention is a total of one or more compounds selected from the group consisting of lophenol compounds and cyclolanostane compounds, more preferably at least 0.0001% by mass, It is preferable to use a composition containing at least 0.0005% by mass, particularly preferably at least 0.001% by mass, as an active ingredient.

The food and drink composition for promoting UCP expression of the present invention is effective for the prevention and / or amelioration of symptoms and diseases caused by the decrease in the activity of UCP.
The present invention is the same as the target for prevention or improvement in the food and drink composition for promoting UCP expression, the target for prevention or improvement of the form of the above-mentioned medicine.

  In addition, the amount of the compound in the food and drink composition for promoting UCP expression is preferably 0.0001 to 100 mg / day, more preferably 0.001 to 50 mg / day, in total, depending on the form. An amount suitable for intake can be also particularly preferably in the range of 0.01 to 10 mg / day. Therefore, the food and drink composition for promoting UCP expression of the present invention preferably contains the above-mentioned compounds in a total amount of preferably 0.0001 to 100 mg / day, more preferably 0.001 to 50 mg / day, particularly preferably 0.01 to 50 mg / day. It is preferably used to take 10 mg / day.

  The food and drink are preferably health functional food. "Health functional food" means a food with the effect of preventing disease or reducing the risk of disease directly or indirectly displayed, and a product package based on scientific basis at the responsibility of the business operator As an indication of gender, it means food that has been submitted to the Consumer Agency. For example, food products sold in the form of food for specified health use, food for functional indication, health supplements and the like are currently mentioned in Japan.

  The form of the food and drink is not particularly limited, but beverages such as soft drinks, carbonated drinks, nutritional drinks, fruit juice drinks, lactic acid bacteria drinks and the like (including concentrated stock solutions of these drinks and powders for preparation) efficiently Particularly preferred from the viewpoint of intake.

  Moreover, as a form of a functional food-drinks, it is also preferable that it is a granular form, a tablet form, or a liquid supplement from the point that the user can grasp | ascertain the intake of an active ingredient easily.

  In addition, such functional food and drink include “for the prevention and / or amelioration of symptoms caused by the decrease in UCP activity”, “for the prevention and / or amelioration of stroke”, “prevention and / or amelioration of sarcopenia”. In order to improve it, to use it for the prevention and / or improvement of muscle weakness associated with aging and aging, and for the prevention and / or improvement of neurodegenerative diseases preferable. That is, the food and drink of the present invention is effective in selecting a compound selected from the group consisting of Compound 1 and Compound 2, for example, for the purpose of “preventing and / or ameliorating muscle weakness associated with aging and aging”. It is preferable to sell as a food and drink for the prevention and / or amelioration of the symptoms caused by the decrease in activity of UCP, which is contained as an ingredient.

The "indication" includes all indications having a function of informing the consumer of the application. That is, any display that can recall or infer the use, regardless of the purpose of the display, the content of the display, the target object to be displayed, the medium, etc., corresponds to the "display".
Further, the phrase "displayed" means that there is a display act to associate and recognize the display and food and drink (product).
It is preferable that the display action is one that allows the consumer to directly recognize the application. Specifically, the application of the application to the product or the package of the food or drink according to the present invention, the advertisement for the product, the price list or the transaction document (including those provided by an electromagnetic method) Can be illustrated.

On the other hand, the content to be displayed (display content) is a display approved by the administration etc. (for example, a display that is approved based on various systems defined by the administration and is performed in a mode based on such approval) Is preferred.
For example, display of health food, functional food and drink, enteral nutritional food, special purpose food, health functional food, food for specified health use, functional food for nutrition, functional indication food, non-commercial goods for medical use etc. it can. In particular, the indication approved by the Consumer Agency, for example, the indication approved by the system for food for specified health, a similar system can be exemplified. Examples of the latter may be labeling as food for specific health, labeling as food for conditional health, labeling indicating that the structure or function of the body is affected, disease risk reduction labeling, etc. In terms of health promotion law enforcement regulations (April 30, 2003 Ministry of Health, Labor and Welfare ordinance No. 86 in Japan, Japan) labeling as food for specified health (especially display of uses of health), and similar Indications can be listed as a typical example.

The wording representing the use is “for the prevention and / or amelioration of symptoms caused by the decrease in activity of UCP”, “for the prevention and / or amelioration of stroke”, “for the prevention and / or amelioration of sarcopenia”, It is not limited to the words "for the prevention and / or amelioration of muscle weakness associated with aging and aging" and "for the prevention and / or amelioration of neurodegenerative diseases", and even other words, It is needless to say that a term expressing an action or an effect that prevents or ameliorates a symptom caused by a decrease in UCP activity is included in the scope of the present invention.
Moreover, in addition to the display of the said application, it is preferable that the food-drinks of this invention also include the display of the said active ingredient, and also the display which shows the relevance of the said application and the said active ingredient.

The said food-drinks can be manufactured by mix | blending the compound chosen from the compound 1 and the compound 2 as an active ingredient. The food-drinks of this invention can be manufactured by, for example, mixing the said compound with food-drinks raw material, and processing it.
Moreover, the said food-drinks process the extract obtained by extracting using the hot water and various solvents, supercritical extraction, subcritical extraction using the well-known plant etc. containing the said compound with the food-drinks raw material It can also be manufactured by doing.

  When the food or drink is in the form of a granular, tablet or liquid supplement, the compound as the active ingredient may be, for example, saccharides such as lactulose, maltitol and lactitol, and other saccharides For example, dextrin, starch etc .; Proteins such as gelatin, soy protein, corn protein etc .; Amino acids such as alanine, glutamine, isoleucine etc .; polysaccharides such as cellulose, gum arabic etc. together with fats and oils such as soybean oil, neutral fatty acid triglyceride etc. It is also preferable to formulate.

  EXAMPLES The present invention will next be described in more detail by way of examples, which should not be construed as limiting the invention thereto.

Production Example 1
(Production of Rophenol Compound (Compound 1))
100 kg of aloe vera gel mesophyll (clear gel part) was liquefied using a homogenizer, to which a mixture of 100 L of ethyl acetate / butanol (3: 1) was added and stirred. After standing overnight, the ethyl acetate / butanol mixture and the aqueous layer were separated to recover an ethyl acetate / butanol mixture. The ethyl acetate / butanol mixture was concentrated under reduced pressure. The mass of the ethyl acetate / butanol mixed solution extract recovered was 13.5 g.
A solution of 13 g of the extract in 1 ml of a mixture of chloroform / methanol (1: 1) is passed through a column packed with 400 g of silica gel 60 (manufactured by Merck) and adsorbed on the column, and then chloroform / Using a methanol mixture (chloroform: methanol = 100: 1, 25: 1, 10: 1, 5: 1, and 1: 1 mixing ratio), stepwise gradient method of increasing methanol concentration Elution was performed, and the eluate was fractionated at each mixing ratio of the mixture. Among these fractions, the presence of the rophenol compound of the present invention in the fraction eluted with chloroform: methanol = 25: 1 was evaluated by normal phase and reverse phase thin layer chromatography (silica gel 60 F 254 manufactured by Merck, and RP-18 F 2543). It confirmed by).
After removing the solvent of this fraction, it is dissolved in 1 ml of a mixture of chloroform / methanol (1: 1), passed through a column packed with 100 g of silica gel 60, adsorbed on the column, and then hexane / ethyl acetate (4 : 1) Elution was performed with 1,100 ml of the mixture. The eluted fractions were collected in the order of 300 ml (fraction A), 300 ml (fraction B) and 500 ml (fraction C).
It was confirmed by normal phase and reverse phase thin layer chromatography that the lophenol compound which is the compound 1 of the present invention was concentrated in fraction A, and further HPLC equipped with Cosmoseal C 18 (manufactured by Nacalai Tesque) Using a mixture of chloroform / hexane (85:15), 4-methylcholest-7-en-3-ol, 4-methylergost-7-en-3-ol, and 4-methyls 1.3 mg, 1.2 mg, and 1 mg of tigmast-7-en-3-ol were obtained, respectively. The structure of each compound was confirmed by mass (MS) analysis and NMR.

Production Example 2
(Production of Cyclolanostane Compound (Compound 2))
250 ml of distilled water, 50 g of sodium hydroxide, 50 ml of isopropanol, 150 ml of ethanol, 150 ml of ethanol and 150 ml of methanol were added to 8.0 g of γ-oryzanol (manufactured by Oryza Oil Co., Ltd.), and heating and reflux were performed for 2 hours using a mantle heater. After the reaction, the reaction solution was added to 1300 ml of water, and the resulting white precipitate was suction filtered to obtain a solid. In order to wash the remaining alkali, the obtained residue was suspended in 1000 ml of water, and suction filtration was performed again. This operation was repeated twice, and the final residue was freeze-dried under reduced pressure to obtain 5.91 g of oryzanol hydrolyzate. The hydrolyzate was purified by HPLC to obtain 2435 mg of cycloartenol and 1543 mg of 24-methylene-9,19-cyclolanostan-3-ol (compound 2).
Next, using the obtained cycloartenol, synthesis of 9,19-cyclolanostan-3-ol (compound 2) was performed.
302 mg of cycloartenol, 150 ml of isopropanol, and 1.0 g of powdered 5% palladium on carbon catalyst were charged, and this was sealed in an autoclave and replaced with nitrogen gas, and then the pressure of hydrogen gas 3 kg / cm ² Introduced while The mixture was heated with stirring. When the temperature reached 50 ° C., the pressure of hydrogen was adjusted to 5 kg / cm ^2, and the reaction was carried out for 6 hours while maintaining the pressure by supplementing the absorbed hydrogen. The reaction solution was filtered to remove the catalyst and concentrated, and then purified by silica gel column chromatography (developing solvent: chloroform 100%) to obtain 275 mg of 9,19-cyclolanostan-3-ol.

[Production Example 3]
(Preparation of a sample to which a mixture of lophenol compound and cyclolanostane compound is added)
4-Methylcholest-7-en-3-ol, 4-Methylergst-7-en-3-ol, and 4-Methylstigst-7-en-3-ol obtained by the above Preparation Example 1 And a rophenol compound and a cyclolanostane compound using 9,19-cyclolanostan-3-ol and 24-methylene-9,19-cyclolanostan-3-ol obtained by Preparation Example 2 A mixture was obtained such that the mass ratio of the lophenol compound and the cyclolanostane compound was 1: 1: (1): rophenol compound (compound 1): cyclolanostane compound (compound 2).
A mixture of a rophenol compound and a cyclolanostane compound was dispersed using propylene glycol (manufactured by Wako Pure Chemical Industries, Ltd.) to prepare a 5000-fold diluted solution. The solution was diluted 100 times with distilled water to prepare a test sample 1.
That is, Test Sample 1 was produced, which contained 0.0002% by mass in total of Compound 1 (rophenol compound) and Compound 2 (cyclolanostane compound).

Example 1
In this example, the action to increase UCP expression of the composition containing Compound 1 and Compound 2 was examined.

(1) Test sample In this example, the test sample 1 obtained in the above-mentioned Production Example 3 was used. In addition, 1% propylene glycol aqueous solution was used as a control sample.

(2) Test method After 6 weeks old C57BL / 6 mice (manufactured by Nippon SLC Co., Ltd.) were preliminarily bred with animal feed D12450B (manufactured by Research Diets, Inc.) for 1 week, animal feed D12492 (Research The sample was switched to Diets, Inc. and bred for 2 weeks. The fed C57BL / 6 mice were divided into a control group and a test sample group so as to have 12 animals in each group, and continuous administration of the test sample was started. Administration of the test sample was carried out by administering test sample 1 to mice at a weight of 200 μL / 10 g per day. On the other hand, to the control group, the same amount of 1% propylene glycol aqueous solution was administered as a test sample.
After 12 weeks from the start of administration of test sample 1, dissection was carried out, and scapula brown adipose tissue and buttock white adipose tissue were collected, and the amount of UCP gene expression was evaluated by quantitative Realtime RT-PCR.
The primer sequences of each gene used in this example are shown below.
UCP1-F: TACCAAGCTGTGCATTGTCCA (SEQ ID NO: 1)
UCP1-R: GCACACAAACATGATGACGTTCC (SEQ ID NO: 2)
UCP2-F: AGCCTACAAGACCATTGCACGAG (SEQ ID NO: 3)
UCP2-R: CAATGGCATTACGGGCAACA (SEQ ID NO: 4)
UCP3-F: TGGAGGAGAGAGGAAATACAGAGG (SEQ ID NO: 5)
UCP3-R: TCCAAAGGCAGAGACAAAGTGA (SEQ ID NO: 6)
36B4 / RPLPO-F: GTGTTTGACAACGGCAGCATTTA (SEQ ID NO: 7)
36B4 / RPLPO-R: GACGCGCTTGTACCCATTGA (SEQ ID NO: 8)

(3) Test results Table 1 shows the results of analysis of UCP1 expression in scapula brown adipose tissue 12 weeks after the start of administration, and Table 2 shows the results of analysis of UCP2 expression in buttock white adipose tissue UCP3 in buttock white adipose tissue The expression analysis results are shown in Table 3. In the table, the value is shown as the mean value of 12 animals ± standard deviation, and the p value in the table shows the significance probability by Student t test.

  Moreover, as a result of similarly confirming the effect also about the test sample which contained 0.0002 mass% of compound 1 alone and the test sample which contained 0.0002 mass% of compound 2 alone, any test sample also Similar to the test sample 1, the expression of UCP was shown to be elevated.

(4) Discussion As shown in Table 1, UCP1 in brown adipose tissue showed a high value in the test sample group as compared to the control group. Thus, it was found that intake of a composition containing a cyclolanostane compound and a lophenol compound increases UCP1 activity.

  As shown in Table 2, compared with the control group, UCP2 in white adipose tissue showed a high value in the test sample group. Thus, it was found that UCP2 activity is increased by ingesting a composition containing a cyclolanostane compound and a rophenol compound.

  As shown in Table 3, UCP3 in white adipose tissue showed high values in the test sample group as compared to the control group. Thereby, it turned out that UCP3 activity increases by ingesting the composition containing a cyclolanostane compound and a rophenol compound.

  From the results of Tables 1 to 3, it was found that the test sample containing 0.0002% by mass of the cyclolanostane compound and the lophenol compound has an effect of enhancing the activity of UCP.

That is, it was recognized that the cyclolanostane compound and the lophenol compound have an effect of enhancing the activity of UCP.
More specifically, 4-methyl cholest-7-en-3-ol, 4-methyl ergost-7-en-3-ol, 4-methyl stigmast-7-en-3-ol, 9, 19 It was recognized that -cyclolanostan-3-ol and 24-methylene-9,19-cyclolanostan-3-ol have the effect of enhancing the activity of UCP.

  And it turned out that the effect | action which improves the activity of UCP is acquired by ingesting a cyclolanostane compound and a rophenol compound 0.0000 mass% or more from the result of an Example.

  In addition, since UCP was increased by ingestion of the test sample containing the cyclolanostane compound and the lophenol compound, UCP was also contained in the composition containing 0.00001% by mass or more of the cyclolanostane compound and the rophenol compound. It turned out that it has the effect of enhancing the activity of

Example 2
A drug having a UCP expression promoting effect consisting of the following composition was produced by the following method.
A mixture containing the lophenol compound prepared in Preparation Example 1 and the cyclolanostane compound prepared in Preparation Example 2 in the ratio of a rophenol compound: cyclolanostane compound = 1: 1 is carboxymethylcellulose (CMC: 2% by mass of a composition containing 0.001% by mass of the mixture prepared by adding and dispersing Daiichi Kogyo Seiyaku Co., Ltd.), 2% by mass of medium-chain fatty acid (MCT: manufactured by Riken Vitamin Co., Ltd.), glycerin 4% by mass fatty acid ester (manufactured by Riken Vitamin Co., Ltd.), 0.5% by mass of saponin (manufactured by Maruzen Pharmaceutical Co., Ltd.), 0.2% of ethanol (manufactured by Nippon Alcohol Sangyo Co., Ltd.), maltitol (Yashihara Co., Ltd.) 1.3% by mass), glycerin (manufactured by NOF Corporation) 78%, and water are further added so that the total amount is 100% by mass, Mixtures of phenolic compounds (Compound 1) and cyclolanostane compound (Compound 2) was prepared syrup formulation containing 0.00002% by weight final concentration.
The agent of the present example is effective for the amelioration of the symptoms caused by the decrease in UCP activity.

[Example 3]
The food-drinks composition which has the UCP expression promotion effect which consists of the following composition was manufactured with the following method.
Containing 4% of a mixture containing the lophenol compound produced in Production Example 1 and the cyclolanostane compound produced in Production Example 2 in the rophenol compound: cyclolanostane compound = 6.1: 3.9 In addition, medium-chain fatty acid (MCT: 2% RIKEN VITMINAL CO., LTD.), Glycerin fatty acid ester (RIKEN VITAMIN CO., LTD.) 4%, saponin (Maruzen Pharmaceutical Co., Ltd.) 0.5%, ethanol A mixture of cyclolanostane compound and rophenol compound by mixing 0.2%, maltitol (made by Hayashibara) 1.3%, glycerin (made by NOF Corporation) 78%, water 10% A food additive containing
A food and drink composition containing 0.00002% by mass of a mixture of a rophenol compound (compound 1) and a cyclolanostane compound (compound 2) by adding the manufactured food additive to a beverage and uniformly mixing Manufactured.

Example 4
Containing 0.2% of the test sample 1 prepared in Preparation Example 3, 2% of medium-chain fatty acid (MCT: manufactured by Riken Vitamin Co., Ltd.), 4% of glycerin fatty acid ester (manufactured by Riken Vitamin Co., Ltd.), saponin (Maruzen) Pharmaceutical Co., Ltd. 0.5%, Ethanol (Nippon Alcohol Industry Co., Ltd.) 0.2%, Maltitol (Hyashibara Co., Ltd.) 1.3%, Glycerin (Nippon Oil Co., Ltd.) 78%, Water 10 % Were mixed to produce a food and drink composition containing a mixture of a cyclolanostane compound and a rophenol compound.

  The food-drinks composition of a present Example has a UCP expression promotion effect.

  The present invention can be used for the prevention and / or amelioration and treatment of symptoms caused by decreased activity of UCP.

Claims (8)

  A UCP expression promoter comprising as an active ingredient one or more compounds selected from the group consisting of rophenol compounds and cyclolanostane compounds.   A UCP expression promoter comprising, as an active ingredient, a composition containing 0.00001% by mass or more of one or more compounds selected from the group consisting of rophenol compounds and cyclolanostane compounds.   The UCP expression promoting agent according to claim 1 or 2, wherein the expression promoting target of the UCP expression promoting agent is UCP2.   The agent for promoting the expression of UCP according to claim 3, which is used for the amelioration of damage to the nervous system, promoting the development of the nervous system, and / or preventing the decrease in brain function.   The UCP expression promoter according to claim 1 or 2, wherein a target of expression promotion of the UCP expression promoter is UCP1 and / or UCP3.   The UCP expression promoter according to claim 5, which is used for the prevention or improvement of sarcopenia.   A food and drink composition for promoting UCP expression, comprising as an active ingredient one or more compounds selected from the group consisting of a rophenol compound and a cyclolanostane compound. A food and drink composition for promoting UCP expression, comprising, as an active ingredient, a composition containing 0.00001% by mass or more of one or more compounds selected from the group consisting of a rophenol compound and a cyclolanostane compound.