JP2007091631A - Anti-helicobacter pylori agent and food and beverage containing the same - Google Patents

Abstract

<P>PROBLEM TO BE SOLVED: To obtain an anti-Helicobacter pylori agent containing an extract of Mekabu (fertile leaf separated from a stem of seaweed) and an extract of alga belonging to the genus Ascophyllum and a food and beverage containing the same. <P>SOLUTION: The anti-Helicobacter pylori agent contains an extract of Mekabu (fertile leaf separated from a stem of seaweed) and an extract of alga belonging to the genus Ascophyllum. The extract of Mekabu (fertile leaf separated from a stem of seaweed) is preferably obtained by extraction with an aqueous solvent and the extract of an algae belonging to the genus Ascophyllum is preferably obtained by extraction with an aqueous solvent. The extract of Mekabu (fertile leaf separated from a stem of seaweed) and the extract of alga belonging to the genus Ascophyllum are preferably a mixed extract obtained by extraction from a mixture comprising Mekabu (fertile leaf separated from a stem of seaweed) and an alga belonging to the genus Ascophyllum. Especially, the mixed extract is preferably obtained by extraction from a mixture containing 5-50 mass% of Mekabu (fertile leaf separated from a stem of seaweed). The food and beverage contains the anti-Helicobacter pylori agent. The food and beverage contains preferably 0.001-20 mass% of the mass of the total of the extract of Mekabu (fertile leaf separated from a stem of seaweed) and the extract of alga belonging to the genus Ascophyllum. <P>COPYRIGHT: (C)2007,JPO&INPIT

Description

  The present invention relates to an anti-pylori agent and food and drink containing the same. In more detail, this invention relates to the anti-pylori agent containing a mekabu extract and an Ascophylum algae extract, and food-drinks containing this.

  It has been pointed out that Helicobacter pylori (hereinafter simply referred to as “H. pylori”) is involved in the onset of diseases such as gastritis, gastrointestinal ulcer and gastric cancer. In order to survive in the epithelium of the gastric mucosa, it is necessary to use a bactericidal agent that is not affected by gastric acid and can penetrate into the epithelium. However, it is mainly composed of antibiotics that can obtain satisfactory results in vivo. There are few drugs to do. Antibiotics are always concerned about the induction of resistant bacteria. For this reason, in recent years, research has been conducted on various components that replace anti-pylori antibiotics. That is, for example, the following Patent Documents 1 to 5 can be mentioned.

JP 07-138166 A International Publication No. 00/20009 Pamphlet Japanese Patent Laid-Open No. 2000-046062 International Publication No. 98/013328 Pamphlet JP 2002-223727 A

  In addition to the anti-pylori agents disclosed in the above patent documents, it is desired to obtain more anti-pylori agents. This makes it possible to obtain a safer and more accurate anti-pylori effect from other types of plants. This invention is made | formed in view of the said actual condition, and it aims at providing the anti-H. Pylori agent containing the mekabu extract and the Ascophylum algae extract, and the food and drink containing this.

The present invention is as follows.
(1) An anti-pylori fungus agent characterized by containing a mekabu extract and an Ascophilum algae extract.
(2) The anti-pylori as described in (1) above, wherein the total amount of the mekabu extract and the Ascophylum algae extract is 0.001 to 20% by mass when the total anti-pylori agent is 100% by mass. Fungus agent.
(3) The anti-pylori agent according to (1) or (2) above, wherein the mechabu extract is an extract with an aqueous solvent.
(4) The anti-pylori agent according to any one of (1) to (3) above, wherein the Ascophilum algae extract is an extract with an aqueous solvent.
(5) The antibacterial extract according to any one of (1) to (4) above, wherein the mechabu extract and the Ascophilum algae extract are a mixed extract extracted from a mixture containing Mekabu and Ascophilum algae. Helicobacter pylori agent.
(6) The anti-pylori agent according to the above (5), which contains 5 to 50% by mass of the mechab when the total of the mechab and the Ascophylum algae is 100% by mass.
(7) A food or drink comprising the anti-pylori agent according to any one of (1) to (6) above.
(8) The food and drink according to (7) above, containing the Mekabu extract and the Ascophyllum algal extract in a total amount of 0.001 to 20% by mass when the entire food and drink is 100% by mass.

The anti-pylori agent of the present invention is a seaweed-derived anti-pylori agent, has high safety and sufficient anti-pylori activity, especially gastritis (chronic gastritis etc.), enteritis, gastric ulcer, intestinal ulcer ( Prevention, suppression, improvement and treatment of diseases such as duodenal ulcers).
When the mekabu extract and the Ascophilum algae extract are contained in a predetermined range, an inexpensive anti-pylori agent can be obtained while exhibiting sufficient anti-pylori activity.
When the mekabu extract is an extract from an aqueous solvent, it can be an inexpensive anti-pylori agent while exhibiting sufficient anti-pylori activity.
When the Ascophylum algae extract is an extract obtained from an aqueous solvent, an inexpensive anti-pylori agent can be obtained while exhibiting sufficient anti-pylori activity.
When the mekabu extract and the Ascophylum algae extract are a mixed extract extracted from a mixture containing Mekabu and Ascophilum algae, it is possible to efficiently obtain an anti-H. Pylori agent that provides sufficient anti-H. Pylori activity. it can.
When mekabu is contained in a predetermined range with respect to the total amount of mekabu and ascophyllum, particularly high anti-pylori activity can be obtained efficiently.
According to the food and drink of the present invention, it is highly safe and has sufficient anti-H. Pylori activity, in particular, prevention of diseases such as gastritis (such as chronic gastritis), enteritis, gastric ulcer, intestinal ulcer (such as duodenal ulcer), Inhibition, improvement and treatment can be performed.
When the mekabu extract and the Ascophilum algae extract are contained in a predetermined range, an inexpensive anti-pylori agent can be obtained while exhibiting sufficient anti-pylori activity.

Hereinafter, the present invention will be described in detail.
[1] Anti-pylori agent The anti-pylori agent of the present invention is characterized by containing a mekabu extract and an Ascophylum algae extract.

The “mechabu extract” is a component extracted from mekabu. The mekabu used for the extraction of this mekabu extract is a pleated spore in the root of wakame, a kind of brown algae. Since the mekabu is a part responsible for the breeding of seaweed, nutrients are condensed.
The “Ascophylum algae extract” is a component extracted from Ascophilum algae. The Ascophilum algae used for extraction of this Ascophilum algae extract is a kind of brown algae, and is a brown alga from the high latitudes, particularly Northern Europe etc. at 60-68 degrees north latitude. Specific examples of the Ascophyllum algae include Ascophyllum Nodosum. There are no particular limitations on the production area of the mekabu and the ascophyllum algae, and in the present invention, mekabu and ascophyllum algae obtained from seaweed produced in various places can be used.

  The mechabu and the Ascophilum algae can be used after washing the harvested water. Furthermore, for example, sun-dried or hot-air dried at an appropriate temperature can be used. These can be subjected to extraction as they are, but for efficient extraction, it is preferable to make mekabu and Ascophyllum algae into string, small pieces or powder and increase the contact area with the solvent during extraction. The diameter and length of the string are not particularly limited, but the diameter is preferably 10 mm or less, particularly 0.5 to 5 mm, more preferably 0.5 to 3 mm, and the length is 300 mm or less, particularly 2 to 200 mm. Preferably there is. Also, the size of the small piece is not particularly limited, but the maximum size is preferably 100 mm or less, particularly 2 to 30 mm. Further, the average particle diameter of the powder is not particularly limited, but is preferably 2 mm or less, particularly 0.1 to 1 mm, and more preferably 0.3 to 0.8 mm. Furthermore, the mechabu and the Ascophylum algae may be subjected to pretreatment such as impurity removal as necessary.

  In the anti-pylori agent of the present invention, the total content of the mekabu extract and the ascophyllum algae extract (hereinafter also simply referred to as “both extracts”) when the total anti-pylori agent is 100% by mass is It is not specifically limited, It is preferable to set it as 0.001 mass% or more (it may be 100 mass%). When both the above extracts are mixed with other components and used, the total content of both extracts is preferably 0.001 to 20% by mass, more preferably 0.005 to 10% by mass, 10 mass% is especially preferable. In addition, for example, when both the above extracts are used dissolved in a solvent, the total content of both extracts is preferably 0.01 mg / ml or more, more preferably 0.1 mg / ml or more, and 0.3 mg / ml or more. Is more preferable, 0.3 to 5.0 mg / ml is still more preferable, and 0.3 to 3.0 mg / ml is particularly preferable.

  In addition, the mekabu extract contained in the anti-pylori agent of the present invention may be an extract with an aqueous solvent or an extract with an oil solvent, and among these, extraction with an aqueous solvent is possible. It is preferable that it is a thing. Further, the Ascophilum algae extract may be an extract with an aqueous solvent or an extract with an oil-based solvent, and among these, an extract with an aqueous solvent is preferable. The extraction solvents for the mekabu extract and the Ascophylum algae extract may be the same or different, but both are preferably aqueous solvents.

  The “aqueous solvent” represents a solvent composed of only water and a solvent composed of water and a component that can be dissolved in water. Components that can be dissolved in water include organic solvents and inorganic compounds. Examples of the organic solvent include monohydric alcohols having 1 to 5 carbon atoms (ethanol, methanol, propanol, isopropanol, butanol, etc.), polyhydric alcohols having 2 to 5 carbon atoms {glycerin, isopropylene glycol, propylene glycol, butylene glycol (1 , 3-butylene glycol and the like}, esters (methyl acetate and the like), ketones (acetone and the like), and the like. Among these, monohydric alcohols having 1 to 5 carbon atoms (preferably 1 to 4 carbon atoms) and / or polyhydric alcohols having 2 to 5 carbon atoms (preferably 1 to 4 carbon atoms) are preferable, and carbon A monohydric alcohol having 1 to 5 (preferably 1 to 4 carbon atoms) is preferable, and a monohydric alcohol having 1 to 2 carbon atoms (methanol and ethanol) is particularly preferable. These organic solvents may use only 1 type and may use 2 or more types together.

Among the above, when a mixed solvent of water and an organic solvent is used, when the total of water and the organic solvent is 100% by mass, the organic solvent is 80% by mass or less (usually 5% by mass or more), and further 50% by mass. Hereinafter, it is particularly preferable that the content be 40% by mass or less. In this range, the extraction efficiency can be particularly increased.
Moreover, when using C1-C5 monohydric alcohol (henceforth only "alcohol") as an organic solvent used for the said mixed solvent, when the sum total of water and alcohol is 100 mass%, alcohol Is preferably 10 to 50% by mass, more preferably 15 to 40% by mass, and particularly preferably 20 to 40% by mass.

  As the inorganic compound, the pH of the extraction solvent such as inorganic compound (buffering inorganic compound) for buffering the extraction solvent such as sodium dihydrogen phosphate, disodium oxyhydrogen, hydrochloric acid, sulfuric acid, sodium hydroxide, etc. Inorganic compounds for adjusting (inorganic compounds for adjusting pH) and the like. Among these, for example, the buffering inorganic compound can be contained in the extraction solvent so as to have a concentration of 0.005 to 0.015 mol. Moreover, the inorganic compound for pH adjustment can be contained in an extraction solvent so that it may become 0.03-0.08 molar concentration. When these inorganic compounds are contained, an extraction promoting action such as an improvement in extraction efficiency and a reduction in extraction time can be obtained.

  The mechabu extract and Ascophyllum algae extract of the present invention may be a mixed extract that is extracted by mixing with another extract, or a single extract that is independently extracted. . When using the extract by mixed extraction among these, the mixed extract extracted from the mixture containing a mekabu and Ascophyllum algae can be used. Furthermore, the extract extracted from the mixture which consists of a mekabu and an Ascophylum algae can be used.

  When a mixture containing mekabu and Ascophilum algae is used for extraction, the content of mekabu and Ascophilum algae contained in this mixture is not particularly limited, and may be appropriately set depending on the required anti-pylori activity, etc. However, when the total of mekabu and the above Ascophilum algae is 100 mass%, mechabu is 5 to 50 mass%, particularly 7 to 40 mass%, more preferably 10 to 30 mass%. Within the above range, particularly excellent anti-pylori activity can be obtained.

  When performing the above-described mixed extraction, the procedure and the like are not particularly limited as long as extraction is performed with an extraction solvent in a state where mekabu and Ascophylum algae coexist. That is, for example, mechabu and Ascophylum algae may be premixed using a corn blender or the like and then used for extraction or may be used without being premixed. In addition, an extraction solvent may be added to an extraction tank in which mechabu and ascophylum algae are housed, and mechabu and ascophyllum algae may be put into the solvent.

  Regardless of mixed extraction or single extraction, the extraction method is not particularly limited, and immersion extraction, stirring extraction, reflux extraction, shaking extraction, ultrasonic extraction, and the like can be used. These may use only one type of extraction method, or may use two or more types in combination. Furthermore, the extraction operation may be performed once, or may be performed a plurality of times (repeating the extraction residue obtained after the extraction operation is repeated a plurality of times).

  Further, the amount of the extraction solvent to be used is not particularly limited, but when the total of Mekabu and Ascophyllum algae and the extraction solvent is 100% by mass, the extraction solvent is 90 to 99% by mass, more preferably 91 to 98% by mass, especially It is preferable that it is 92-97 mass%. Within this range, an anti-pylori agent having sufficient anti-pylori activity can be obtained.

Furthermore, the extraction conditions for performing the extraction are not particularly limited. That is, for example, the extraction temperature is not particularly limited, and may be room temperature extraction or heat extraction. In the room temperature extraction, for example, the extraction object can be extracted by being immersed in an extraction solvent having a temperature of 10 to 35 ° C. (further 15 to 30 ° C.). In addition, in heat extraction, it depends on the type of solvent, etc. (in the case of using a mixed solvent containing an organic solvent, it is preferably used below the boiling point of the organic solvent). It can be extracted by being immersed in an extraction solvent having a temperature of 50 to 95 ° C., particularly 60 to 90 ° C. Further, the extraction may be performed at a constant temperature or the temperature may be changed. When the extraction solvent is an aqueous solvent, particularly when it is water, heat extraction is preferred, and the temperature of the extraction solvent is 40 to 100 ° C., more preferably 50 to 100 ° C., even more preferably 60 to 100 ° C., particularly 65 to 65 ° C. The temperature is preferably 95 ° C, more preferably 70 to 90 ° C.
When the extraction temperature is in the above range, an extract containing an anti-H. Pylori component can be efficiently obtained in a short time, and a decrease in the anti-H. Pylori activity of the extract can be suppressed. The reason for this is not clear, but it is thought that one of the reasons is that the decomposition of the compound having anti-pylori activity is suppressed.

Moreover, although the pH of an extraction solvent is not specifically limited, For example, it can be 3-10 (further 4-9, especially 5-8). Further, the extraction pressure is not particularly limited, and may be normal pressure, pressurization, or reduced pressure.
Furthermore, the extraction time is not particularly limited. The extraction time may be an appropriate time depending on other extraction conditions such as the extraction temperature. For example, 0.5 to 5 days (further 0.5 to 6 hours, even more 1 to 5 hours, particularly 1. 5 to 4 hours). If the extraction time is within the above range, an extract having sufficient anti-pylori activity can be obtained.

  More specifically, as the extraction condition, when performing heat extraction, the extraction temperature may be 40 to 100 ° C., and the extraction time may be 0.5 to 6 hours. Moreover, it is preferable that extraction temperature is 50-95 degreeC, and extraction time is 1-5 hours, extraction temperature is 60-90 degreeC, and extraction time is 1.5-4 hours more. preferable. When performing normal temperature extraction, extraction temperature can be 10-35 degreeC (further 15-30 degreeC), and extraction time can be 0.5 hour-5 days.

  Furthermore, a combination of the amount of the extraction solvent (mass ratio of the extraction solvent when the total of Mechabu and Ascophyllum algae and the solvent is 100% by mass) and the extraction conditions described above is 90 to 99. The mass%, the extraction temperature can be 40 to 100 ° C., and the extraction time can be 0.5 to 6 hours. Further, it is preferable that the amount of the extraction solvent is 92 to 97% by mass, the extraction temperature is 50 to 95 ° C., and the extraction time is 1 to 5 hours. In this case, the solvent is preferably an aqueous solvent, and water is particularly preferable.

  The extract residue after the extraction (mechabu and Ascophilum algae after extraction) and the extract (including the mekabu extract and / or Ascophyllum algae extract) are usually separated and the anti-antibody of the present invention is separated. Used as a Helicobacter pylori agent. Although the separation method in this case is not particularly limited, it can be separated by a filter press, filtration (pressurization, normal pressure) or the like. The extract separated from the extraction residue can be used as it is as the anti-pylori agent of the present invention. Further, the extracted liquid separated from the extraction residue can be used after further removing the solvent contained therein. The method for removing the solvent from the extract is not particularly limited, and can be performed by, for example, spray drying, evaporation, freeze drying, or the like. The solid content (mechabu extract and / or Ascophyllum algae extract) collected from the extract may be used as it is, or further purified. That is, after this solid content is dissolved in water and / or an organic solvent or the like, filtration is performed to remove impurities and the like, and then the solvent is removed for purification. Furthermore, a sterilization process etc. can be given as needed.

  The anti-pylori agent of the present invention is not particularly limited in its form as long as it contains a mekabu extract and an Ascophilum algae extract. For example, the anti-pylori agent of the present invention can be liquid, solid, powder, granule, granulated granulation, and the like. The liquid material is, for example, a solid or powder dried by a known method such as freeze-drying, dissolved or dispersed in water or an organic solvent such as ethanol, propylene glycol and 1,3-butylene glycol, or a mixed solvent thereof. Can be obtained.

Moreover, the anti-pylori agent of this invention can be utilized as a chemical | medical agent, food-drinks, etc. which have anti-pylori activity. The medicine includes a medicine and a quasi drug. When used as this medicine, tablets, pills, capsules, powders, granules, syrups, injections, suppositories, and the like can be used.
Furthermore, the anti-H. Pylori agent of the present invention can impart anti-H. Pylori activity to beverages and foods when added to various beverages and foods. That is, the anti-H. Pylori agent of the present invention can be used as an additive for food and drink to impart anti-H. Pylori activity to beverages and foods.
The anti-pylori agent of the present invention can be used for the purpose of prevention, suppression, amelioration, treatment, or cure of various diseases such as gastritis (chronic gastritis, etc.), enteritis, gastric ulcer, intestinal ulcer (duodenal ulcer etc.), etc. .

  Moreover, the anti-pylori agent of this invention may contain other components other than the said extract, unless the effect of this invention is inhibited. Other ingredients include molding agents, binders, disintegrants, disintegration inhibitors, lubricants, carriers, solvents, extenders, tonicity agents, emulsifiers, suspending agents, dispersants, thickeners, coatings. Agents, absorption promoters, coagulants, preservatives (stabilizers, moisture-proofing agents, anti-coloring agents, antioxidants, etc.), flavoring agents, flavoring agents, coloring agents, antifoaming agents, soothing agents, antistatic agents, and A pH adjuster etc. are mentioned. These may use only 1 type and may use 2 or more types together.

  Furthermore, the administration method of the anti-pylori agent of the present invention is not particularly limited and may be oral administration or other administration methods such as injection administration (intravenous injection, intramuscular injection, subcutaneous injection, etc.). Also good. These administration methods may use only 1 type and may use 2 or more types together. Of these, oral administration is preferred. The dose is preferably adjusted according to age, body weight, symptom, therapeutic effect, administration method, and the like, and is usually in the range of 1 to 1000 mg at a time per day in terms of solid per adult. It can be administered several times. Since the dose varies depending on various conditions, a dose smaller than the above dose may be sufficient, or it may be necessary to administer beyond the above dose range. For example, when used as a medicine, when the total amount of the medicine is 100% by mass, the anti-pylori agent of the present invention (in terms of solids) is 0.001 to 20% by mass (further 0.005 to 10% by mass, especially 0). .01 to 10% by mass).

  The anti-H. Pylori agent of the present invention can exhibit superior anti-H. Pylori characteristics as compared to the case of using only the mekabu extract or only the Ascophilum algae extract. That is, anti-H. Pylori characteristics can be improved by using each extract in combination as compared with a single use. The reason is not clear.

[2] Food and drink containing anti-pylori agent The food and drink of the present invention contains the anti-pylori agent of the present invention. That is, the anti-pylori agent of the present invention can be used in foods and drinks. For example, the anti-pylori agent of the present invention may be blended directly into a beverage, or it may be blended into the raw materials of solid foods such as biscuits, cream-like and jam-like semi-fluid foods, and gel-like foods. It can be provided as gastroenteritis-preventing foods, gastrointestinal ulcer-preventing foods, gastric cancer-preventing foods, health foods, functional foods, and the like containing the Helicobacter pylori agent. Further, the anti-pylori agent of the present invention is dissolved in, for example, alcohols such as fats and oils, ethanol, propylene glycol and glycerin, and mixtures thereof, and then blended into a beverage, or a solid food, semi-liquid food or It can also be blended in gel food. Furthermore, if necessary, gum arabic and dextrin that act as a binder are blended to form a granule, etc., which can be blended into a beverage, or blended into a solid food, semi-fluid food or gel food. it can.

  The kind of food and drink containing the anti-pylori agent is not particularly limited, and may be any of solid foods, cream-like and jam-like semi-fluid foods, gel-like foods and beverages. More specifically, the food or drink of the present invention can be, for example, a food or drink that exhibits a specific health effect, or a functional food or drink that takes advantage of the function of the biological adjustment component. Specific examples of the food and drink of the present invention include liquor, carbonated beverages, fruit beverages, coffee, tea, tea, lactic acid bacteria beverages, yogurt, ice cream, rice cake, gum, confectionery, bread, and noodles.

  In the food and drink of the present invention, the compounding amount of the anti-pylori agent of the present invention is not particularly limited. Ingestion as a health food or functional food is usually for the purpose of disease prevention, health maintenance, etc., so adjust the compounding amount of the anti-pylori agent of the present invention according to age, weight, sex, etc. It is preferable. When the total amount of the food and drink of the present invention is 100% by mass, the compounding amount (in terms of solid) of the anti-pylori agent of the present invention is 0.001 to 20% by mass, particularly 0.005 to 10% by mass, and further 0 It is preferable that it is 0.01-10 mass%.

Specifically, the following prescription is mentioned as food / beverage prescription of this invention, for example. The following purified dry powder of the anti-pylori agent of the present invention is a powder obtained by freeze-drying an extract and then purifying it. The food and drink of the present invention produced by the following prescription is effective for gastroenteritis prevention, gastrointestinal ulcer prevention, gastric cancer prevention and the like, but this action effect limits the technical scope of the food and drink of the present invention. Not the purpose.
(1) Soft capsule brown rice germ oil 87.0 mass%
Emulsifier 12.0% by mass
Anti-H. Pylori agent (purified dry powder) 1.0% by mass
Total 100% by mass

(2) Soft drink
Fructose glucose liquid sugar 30.0% by mass
Emulsifier 0.5% by mass
Anti-H. Pylori agent (purified dry powder) 0.05% by mass
Fragrance Trace amount purified water Total balance 100% by mass

(3) Tablet lactose 54.0% by mass
Crystalline cellulose 30.0 mass%
Starch degradation product 10.0% by mass
Glycerin fatty acid ester 5.0% by mass
Anti-H. Pylori agent (purified dry powder) 1.0% by mass
Total 100% by mass

(4) Tablet confectionery sugar 76.4% by mass
Glucose 19.0% by mass
Sucrose fatty acid ester 0.2% by mass
Anti-H. Pylori agent (purified dry powder) 0.5% by mass
Purified water 3.9% by mass
Total 100% by mass

Hereinafter, the present invention will be described specifically by way of examples.
[1] Mekabu and Ascophyllum algae used Mekabu (Korean); Wakame (scientific name "Undoria pinnatifida") root of "spore-shaped" dried material cut into 1-2 mm width was used.
Ascophyllum algae (from Northern Europe); a dried product of Ascophyllum nodsum (scientific name “Ascophyllum nodosum”) was pulverized into powder having a size of 30 to 40 mesh (0.43 to 0.60 mm).

[2] Preparation of Practical Product and Comparative Product (1) Preparation of Anti-H. Pylori Agent 10 g of the above mekabu and 40 g of the above Ascophyllum algae were weighed, and both were put into a glass container equipped with a stirrer having an internal volume of 2 liters. Next, 1 liter of water was put into this container, and then the container was heated to 80 ° C., and extraction was performed by holding at 80 ° C. for 2 hours with occasional stirring. Subsequently, the obtained extract is subjected to suction filtration using a G200 glass filter (manufactured by Toyo Roshi Kaisha), and the filtrate is concentrated under reduced pressure. An agent was obtained.

(2) Preparation of reagents i) Example 1
Example 1 was obtained by encapsulating 100 mg of the anti-pylori agent obtained in the above [2] (1) and 100 mg of lactose in a gelatin capsule.
ii) Example 2
Example 2 was obtained by encapsulating only 750 mg of the anti-pylori agent obtained in [2] (1) above in a gelatin capsule.
iii) Comparative Example 1
Only 200 mg of lactose was enclosed in a gelatin capsule to obtain Comparative Example 1 (placebo).

[3] Activity evaluation of anti-H. Pylori (1) Selection of carriers of H. pylori Serum was isolated from blood collected from 34 subjects who obtained consent, and an anti-H. Pylori antibody detection kit (available from Mizuho Media Co., Ltd., product name “ The presence or absence of anti-H. Pylori antibodies was determined using “Minnitreed pylori antibody”). As a result, 15 out of 34 people were positive. In other words, these 15 people have anti-H. Pylori antibodies and are considered to have had an opportunity to infect H. pylori until now.
Thereafter, for 15 subjects who were positive for the above-mentioned anti-H. Pylori antibody, according to the prescription using a ¹³ C urea breath test agent (Otsuka Pharmaceutical Co., Ltd.) and a breath gas analyzer (Otsuka Electronics Co., Ltd.). It was confirmed whether or not the taken urea was decomposed into carbon dioxide. As a result, it was confirmed that 9 out of 15 people decomposed urea and were H. pylori carriers.

(2) Reagent use For 9 persons who were found to be H. pylori carriers in [3] (1) above, Example 1 (containing 100 mg of anti-H. Pylori), Example 2 (containing 750 mg of anti-H. Pylori) ), Comparative Example 1 (placebo) was administered once a day for 14 days.

^{(3) 13} C urea breath test the ¹³ CO ₂ detecting the amount of change rate by ¹³ C urea breath test measured after administration 14 days for ¹³ CO ₂ detected amount of ¹³ C urea breath test measured before administration of each reagent The average value of the increase / decrease rate was calculated. The amount of ¹³ CO ₂ detected before reagent administration was: placebo group: anti-H. Pylori agent 100 mg / day intake group: anti-H. Pylori agent 750 mg / day intake group = 1.04: 1.00: 1.04 There was little difference between each group.
As a result, the average value in the placebo group was 115% of that before administration. In addition, the average value of the anti-H. Pylori agent 100 mg / day intake group was 85% of that before administration. Furthermore, the average value of the anti-pylori agent 750 mg / day intake group was 72% of that before administration. The results are shown as a graph in FIG.

(4) Effects of Examples Literature “Examination of the effect of gastric mucosal tissue findings on ¹³ C urea breath test in Helicobacter pylori positive cases” (Iijima, 8 others, Japanese Society of Gastroenterology, Japanese Gastroenterological Society, January 1998, 95th volume, No. 1, as shown in ^{p.18-25), 13} CO ₂ detected amount of ¹³ C urea breath test is correlated with H. pylori amount of colonization.
From the results of [3] and (3) above, the placebo group to which placebo (lactose) was administered increased 115% and ¹³ CO ₂ detection amount, while the anti-pylori agent 100 mg / day intake group had 85 It can be seen that it is reduced to 72% in the group receiving 750 mg / day of anti-pylori agent. That is, it can be seen that the number of H. pylori can be reduced by using this H. pylori agent. Furthermore, it can be seen that this reduction in H. pylori is more effective as the dose of H. pylori is increased.

  The present invention can be used in a wide range of applications such as health drinks, health foods, health foods and pharmaceuticals. For example, the anti-pylori agent of this invention can be mix | blended with a drink, and it can be set as an anti-pylori health drink. The pharmaceutical preparation (tablet, capsule, syrup, injection, etc.) containing the anti-pylori agent of the present invention can be administered orally or by intramuscular injection, intravenous injection or arterial injection.

It is a graph which shows the effect of the anti-pylori agent concerning an Example.

Claims (8)

  An anti-pylori fungus agent comprising a mekabu extract and an Ascophyllum algae extract.   The anti-pylori agent of Claim 1 which contains 0.001-20 mass% in total of the said mekabu extract and the said Ascophylum algae extract when this anti-pylori agent whole is 100 mass%.   The anti-pylori agent according to claim 1 or 2, wherein the mechabu extract is an extract with an aqueous solvent.   The anti-pylori agent according to any one of claims 1 to 3, wherein the Ascophilum algae extract is an extract with an aqueous solvent.   The anti-H. Pylori agent according to any one of claims 1 to 4, wherein the mechabu extract and the Ascophylum algae extract are mixed extracts extracted from a mixture containing Mekabu and Ascofilum algae.   The anti-pylori agent of Claim 5 which contains 5-50 mass% of this mekabu when the sum total of the said mekabu and the said Ascophylum algae in the said mixture is 100 mass%.   A food or drink comprising the anti-pylori agent according to any one of claims 1 to 6.   The food and drink according to claim 7, comprising 0.001 to 20% by mass in total of the mekabu extract and the Ascophyllum algal extract when the total amount of the food and drink is 100% by mass.

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