The invention relates to an agent for preventing, improving or treating hypertension, which exhibits a hypotensive effect, inhibits the rise of blood pressure and improves hypertension, and food for preventing or improving hypertension, which does not become a burden in daily intake, has a higher antihypertensive effect and is useful as a diet during treatment for patients of hypertension. The agent for preventing, improving or treating hypertension contains the following components (A) and (B):

• (A) a compound selected from the group consisting of caffeic acid, chlorogenic acid and ferulic acid, and esters and pharmaceutically acceptable salts thereof; and
• (B) a component selected from the group consisting of central nervous system stimulating components, food fibers, extracts of perennial evergreen leaves of the genus Camellia, Theaceae, or Eucommia ulmoides Oliver, Eucommiae, organic acids having a molecular weight of 60 to 300 (excluding citric acid) and pharmaceutically acceptable salts thereof, and sugar alcohols.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

The component (A) used in the present invention may be a product chemically synthesized. However, an extract of a natural substance containing this component, particularly, a plant may be used. Examples of the plant include coffee, onion, radish, lemon, MOROHEIYA, Cnidium officinale Makino, Angelica acutiloba Kitagawa, pine, Captis japonica Makino, asafetida, sugarcane, corn, barley and rice.

Caffeic acid and chlorogenic acid may also be extracted from a plant such as green beans of coffee, leaves of nandin or an immature fruit of apple. For example, an acid obtained by extraction of seeds of Coffea arabica LINNE, Rubiaceae with hot water or with an aqueous solution of ascorbic acid or citric acid under heating may be used.

Ferulic acid is a compound contained, as an ester thereof, in natural substances, particularly plants such as rice and adlay and may be obtained as a purified product from such a plant or a synthesized product industrially obtained. A ferulic ester is obtained in a hydrous ethanol fraction after rice bran oil obtained from rice bran is partitioned with hydrous ethanol and hexane at room temperature under weakly alkaline conditions. Ferulic acid can be obtained by hydrolyzing the ferulic ester obtained by the above-described process with sulfuric acid with heating under pressure and purifying the resultant hydrolyzate or by culturing Pseudomonas in a medium containing clove oil from buds and leaves of Syzygium aromaticum MERRILL et PERRY, Myrtaceae by steam distillation, or eugenol obtained by purifying the clove oil and subjecting the medium to isolation and purification. When ferulic acid is prepared by chemical synthesis, it may be prepared by, for example, a condensation reaction of vanillin and malonic acid (Journal of American Chemical Society, 74, 5346, 1952).

Incidentally, stereoisomers exist in caffeic acid, chlorogenic acid, ferulic acid or pharmaceutically acceptable salts thereof. However, pure stereoisomers or a mixture thereof may be used in the present invention. The term "chlorogenic acid" in the present specification means chlorogenic acid or a derivative thereof and designates 3-caffeoylquinic acid, 4-caffeoylquinic acid, 5-caffeoylquinic acid, 3,4-dicaffeoylquinic acid, 3,5-dicaffeoylquinic acid, 4,5-dicaffeoylquinic acid, 3-feruloylquinic acid, 4-feruloylquinic acid, 5-feruloylquinic acid, 3-feruloyl-4-caffeoylquinic acid or a mixture thereof.

Esters of caffeic acid, chlorogenic acid and ferulic acid include those naturally contained in natural substances, particularly, plants, those obtained by conversion by a chemical treatment upon extraction and/or fractionation and those chemically modified. Specific examples thereof include esters with an alcohol having 1 to 40 carbon atoms, i.e., ester compounds with a linear or branched alkyl or alkenyl alcohol, allyl alcohol, terpene alcohol, sterol or trimethylsterol, and esters with plant sterol. As with ferulic acid, their corresponding esters of caffeic acid and chlorogenic acid may be used.

The solubility of caffeic acid, chlorogenic acid and ferulic acid in water can be improved by providing them in the form of a pharmaceutically acceptable salt, and their physiological effectiveness can be enhanced. Examples of a basic substance used for forming such a salt include inorganic bases such as alkali metal or alkaline earth metal hydroxides, for example, such as lithium hydroxide, sodium hydroxide, potassium hydroxide, magnesium hydroxide and calcium hydroxide; and ammonium hydroxide; and organic bases, such as basic amino acids such as arginine, lysine, histidine and ornithine; and monoethanolamine, diethanolamine and triethanolamine, with the alkali metal or alkaline earth metal hydroxides being particularly preferred. The agents according to the present invention may be formulated either by preparing such a salt and adding the salt to other components, or by separately adding a salt-forming component and a component to be formed into a salt to other components to react them in the formulation system.

Two or more of the above-described compounds may be used in combination as the component (A) according to the present invention.

In the agent according to the present invention for preventing, improving or treating hypertension, the component (A) may be contained in a proportion of 0.001 to 5% by weight (hereinafter indicated merely by "%"), preferably 0.005 to 5%, more preferably 0.005 to 1%, particularly preferably 0.01 to 1%.

As the component (B) used in the present invention, the central nervous system stimulating components serve to stimulate the central nervous system to induce an exciting effect and are preferably selected from the group consisting of heat components of ginger, red pepper, pepper and the like. Ginger, red pepper and pepper are known as spice.

As ginger, red pepper and pepper, plants belonging to Zingiberaceae, Capsicum and Piperaceae, respectively, are used. With respect to the heat components of these plants, cinerol, zingerone, zingerol, shogaol and the like are contained in a proportion of 0.6 to 10% in ginger, capsaicin and the like are contained in a proportion of about 20% in red pepper, and piperine or the like are contained in a proportion of about 6 to 13% in pepper. These heat components may be either extracts obtained by solvent extraction making use of an organic solvent or the like, or commercially available products. Two or more of these heat components may be used in combination.

When the component (B) is a central nervous system stimulating component, it is preferably contained in a proportion of 0.001 to 1%, particularly 0.005 to 0.5% in the agent according to the present invention for preventing, improving or treating hypertension.

Specific examples of the food fibers as the component (B) used in the present invention include wheat bran composed of exodermis (testa and embryo) prepared by sieving in a milling process of wheat, beet fibers prepared by sieving after grinding of beet pulp, corn fibers prepared by purifying an exodermis division obtained from a wet milling process of corn flour, apple fibers prepared by drying pulp (residue after squeezing of juice, and the like) derived from an apple fruit, cellulose prepared by hydrolyzing pulp and then purified and drying the hydrolyzate, hardly digestible dextrin prepared by partially hydrolyzing starch, further hydrolyzing the partial hydrolyzate with amylase and then decoloring and desalting the hydrolyzate, a decomposed product of guar gum prepared by subjecting guar gum taken out of guar, which is a leguminous plant in an Indian region, to an enzymatic treatment, thyrium testa prepared by grinding testa and exodermis of a plant of Plataginaceae, alginic acid extracted from tang or low molecular sodium alginate prepared by heating and hydrolyzing alginic acid to lower the molecular weight of alginic acid, thereby enhancing the solubility thereof, chitin which is a basic polysaccharide purified by treating a crab shell or the like, or chitosan obtained by leaving the acetyl groups in chitin to make soluble in an acid solution, glucomannan purified by grinding a tuberous root of devil's-tongue to remove starch and washing the resultant devil's-tongue flour with alcohol or water, and lignin which is a phenolic high molecular compound prepared as it is from pulp, hull or bran of cacao or other plants, or from a product obtained by subjecting it to a physiochemical treatment or chemical pretreatment.

Carrageenan, agar, xanthan gum, durane gum, pullulan, pectin, methyl cellulose, which are generally used in food, may also be mentioned.

As the food fibers, are particularly preferred chitosan, lignin, hardly digestible dextrin, alginic acid and low molecular sodium alginate. Two or more of these food fibers may be used in combination.

When the component (B) is food fiber, a drink or food is preferably provided.

When the component (B) is food fiber, it is preferably contained in a proportion of 0.1 to 20%, particularly 0.5 to 10% in the agent according to the present invention for preventing, improving or treating hypertension.

Examples of the extracts of perennial evergreen leaves of the genus Camellia, Theaceae as the component (B) used in the present invention include parched (Chinese style) green tea and roasted (Japanese style) green tea as unfermented tea, HOSHU tea and oolong tea as semi-fermented tea, and black tea (leaf, broken, etc.) as fermented tea.

Examples of the extract of Eucommia ulmoides Oliver include those produced by subjecting leaves collected from Eucommia ulmoides Oliver, Eucommiae to solar drying and roasting.

These extracts are preferably extracts with water or an organic solvent. Examples of the organic solvent include methanol, ethanol, acetic acid, ethyl acetate, n-hexane, acetone, benzene, petroleum ether and chloroform. Extracts with ethanol or water are more preferred. The extracts may be used as it is. However, concentrates obtained by partially removing the solvent, or powders obtained by removing the solvent may be used. Two or more of these extracts may be used in combination. The extracts of Eucommia ulmoides Oliver and oolong tea are preferred.

A preferred combination with the component (A) includes a combination of ferulic acid and the extract of oolong tea or Eucommia ulmoides Oliver, and a combination of ferulic acid and the extract of oolong tea is more preferred from the viewpoint of easy drinking in view of continuous use or intake.

When the component (B) is one of these extracts, it is contained in a proportion of 0.1 to 10%, particularly 1 to 5% in terms of solids in the agent according to the present invention for preventing, improving or treating hypertension.

Examples of the organic acids having a molecular weight of 60 to 300 as the component (B) used in the present invention include carboxylic acids, hydroxycarboxylic acids, polycarboxylic acids, keto-carboxylic acids and the like from the viewpoint of structure, and specific examples thereof include acetic acid, lactic acid, citric acid, gluconic acid, fumaric acid, α-ketoglutaric acid, succinic acid, glycolic acid, malic acid, tartaric acid, pyruvic acid and malonic acid. As the organic acids, are preferred other organic acid than citric acid.

Those naturally contained in natural substances, particularly, plants, those converted by a chemical treatment upon extraction and/or fractionation and those chemically modified are also included. Examples of those derived from the natural substances include brewed vinegar prescribed in the Japanese Agricultural Standard and extracts thereof. The term "brewed vinegar" as used herein means vinegar made by acetic acid fermentation, and specific examples thereof include grain vinegar using rice or other grains as a raw material, for example, grain vinegar called "black vinegar" made by stationary brewing by a single-stage fermentation making use of brown rice and koji as raw materials, fruit vinegar making use of apple, grape or any other fruit, and other brewed vinegar than grain vinegar and fruit vinegar. Fruit juices or extracts thereof may also be used. Specific examples thereof include juices of fruits such as orange, mandarin orange, apple, grape, pineapple, peach, grapefruit, lemon, Japanese pear, pear, Japanese apricot, navel orange, strawberry, passion fruits, melon, lime, guava, apricot, SHIKUWASSHA, kabosu orange, shaddock, iyokan orange, hassaku orange, cranberry, banana, Japanese plum, mango, kiwi fruit, persimmon and ASERORA, mixed juices and concentrates thereof, and extracts thereof with water, ethanol, methanol, acetic acid, chloroform, dichloromethane, ethyl acetate, n-hexane, acetone, benzene, petroleum ether, ether or the like. Extracts with water or ethanol are particularly preferred.

Two or more of these organic acids may be used in combination.

When the component (B) is an organic acid having a molecular weight of 60 to 300, it is contained in a proportion of 0.0005 to 10%, particularly 0.001 to 6% in the agent according to the present invention for preventing, improving or treating hypertension.

Examples of the sugar alcohols as the component (B) used in the present invention include those naturally contained in natural substances, particularly, plants, those converted by a chemical treatment upon extraction and/or fractionation and those chemically modified. Specific examples of the sugar alcohols used include those obtained by reducing the carbonyl groups in monosaccharides, oligosaccharides, polysaccharides and the like to convert them to their corresponding alcohols. Specific examples of monosaccharide alcohols include erythritol which is a sugar alcohol of a tetrose, xylitol from a pentose, and sorbitol and mannitol from a hexose, which are selected by fermentationally decomposing glucose with yeast. Specific examples of oligosaccharide alcohols include parathinit (reduced parathinose), maltitol (reduced maltose) and lactitol of disaccharide sugars, and branched oligosaccharide alcohols. Specific examples of polysaccharide alcohols include reduced dextrin used as reduced starch syrup.

Among these, erythritol, xylitol, maltitol, parathinit, reduced dextrin and branched oligosaccharide alcohols are preferred.

Two or more of these sugar alcohols may be used in combination.

When the component (B) is a sugar alcohol, it is contained in a proportion of 0.1 to 70%, particularly 1 to 50% in the agent according to the present invention for preventing, improving or treating hypertension.

When the agent according to the present invention for preventing, improving or treating hypertension is used as a medicine, a pharmaceutically acceptable carrier may be added to the above-described active components to prepare an oral or parenteral composition. Forms of the oral composition include tablets, granules, grains, pills, powder, capsules (including hard capsules and soft capsules), troches, chewable preparations and solutions (drinks). On the other hand, forms of the parenteral composition include intravenously administering preparations such as injections, suppositories, and external skin care preparations.

When the agent according to the present invention for preventing, improving or treating hypertension is used as a food, other food stuffs may be added to the active ingredients of the components (A) and (B). Examples of the food include drinks and foods, and foods for specific health, such as drinks such as juice and coffee; liquid foods such as soup; emulsion or paste foods such as milk or curry; semisolid foods such as jelly or gumi; solid foods such as gum, bean curd or supplement; powdered foods; and oil-containing foods such as margarine, mayonnaise and dressing. Drinks are particularly preferred.

The effective dose of the agent according to the present invention for preventing, improving or treating hypertension per day for an adult (body weight: 60 kg) is as follows:

When the component (B) is a central nervous system stimulating component, caffeic acid, chlorogenic acid, ferulic acid or a pharmaceutically acceptable salt thereof is preferred as the component (A). The component (A) is preferably ingested in a dose of 0.001 to 10 g, particularly 0.01 to 5 g, while the central nervous system stimulating component is preferably ingested in a dose of 0.0001 to 1 g, particularly 0.001 to 0.5 g.

When the component (B) is food fiber, the component (A) is preferably ingested in a dose of 0.001 to 10 g, particularly 0.005 to 5 g, and the food fiber is preferably ingested in a dose of 0.1 to 50 g, particularly 1 to 10 g.

When the component (B) is an extract of perennial evergreen leaves of the genus Camellia, Theaceae, or Eucommia ulmoides Oliver, Eucommiae, the component (A) is preferably ingested in a dose of 0.001 to 10 g, particularly 0.005 to 5 g, and the extract is preferably ingested in a dose of 0.01 to 50 g, particularly 0.05 to 10 g in terms of solids.

When the component (B) is an organic acid having a molecular weight of 60 to 300 or a pharmaceutically acceptable salt thereof, the component (A) is preferably ingested in a dose of 0.0001 to 5 g, particularly 0.0005 to 1 g in terms of ferulic acid, and the organic acid or the like is preferably ingested in a dose of 0.0001 to 5 g, particularly 0.0005 to 1 g in terms of citric acid.

When the component (B) is a sugar alcohol, the component (A) is preferably ingested in a dose of 0.001 to 10 g, particularly 0.005 to 5 g, and the sugar alcohol is preferably ingested in a dose of 0.1 to 50 g, particularly 1 to 20 g.
 

Claim 1 of 20 Claims

1. A method for treating hypertension comprising:

administering a composition consisting essentially of:

(A) an isolated chlorogenic acid, or an ester or salt of an isolated chlorogenic acid; and

(B) an organic acid having a molecular weight ranging from 60 to 300 or a pharmaceutically acceptable salt thereof,

wherein said organic acid is lactic acid.

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