JPH0753393A - Arteriosclerosis-inhibiting agent and food or medicine containing the same - Google Patents
Arteriosclerosis-inhibiting agent and food or medicine containing the sameInfo
- Publication number
- JPH0753393A JPH0753393A JP5227982A JP22798293A JPH0753393A JP H0753393 A JPH0753393 A JP H0753393A JP 5227982 A JP5227982 A JP 5227982A JP 22798293 A JP22798293 A JP 22798293A JP H0753393 A JPH0753393 A JP H0753393A
- Authority
- JP
- Japan
- Prior art keywords
- arteriosclerosis
- extract
- inhibiting agent
- food
- inhibitor
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
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Links
Abstract
Description
【0001】[0001]
【産業上の利用分野】本発明は動脈硬化抑制剤、及びこ
れを含む食品、又はこれを含む循環器疾患治療用の医薬
組成物に関する。FIELD OF THE INVENTION The present invention relates to an arteriosclerosis inhibitor, a food containing the same, or a pharmaceutical composition containing the same for treating cardiovascular diseases.
【0002】[0002]
【従来の技術】近年、食生活の欧米化が進むにつれて、
国民一人あたりの脂肪摂取量も増加し続けており、中で
も、若年層に於ける総脂肪摂取量の増加と全年齢層に於
ける動物性脂肪摂取量の増加が著しい。このため、過度
に摂取された脂肪によって血中脂質のバランスが崩れた
り、高脂血症が引き起こされたりする。これらが引き金
となって動脈硬化をはじめとする循環器系の成人病にか
かる人が多く、また、循環器系成人病の若年化現象を招
き、大きな社会問題の1つとなっている。2. Description of the Related Art In recent years, as westernization of eating habits has advanced,
The amount of fat intake per capita has continued to increase, and in particular, the increase in total fat intake in young people and the increase in animal fat intake in all age groups are remarkable. For this reason, excessive intake of fat may upset the balance of blood lipids or cause hyperlipidemia. Many of these people are triggered by adult diseases of the circulatory system such as arteriosclerosis, and the aging phenomenon of adult diseases of the circulatory system is caused, which is one of the major social problems.
【0003】このような循環器系成人病の増加を防ぐた
めには、動脈硬化の原因となる高脂血症等の血中脂質の
バランスを改善することが必要であり、その方法として
は、従来より、リノール酸等の多価不飽和脂肪酸を摂取
する方法や、クロロフィブレートやニコチン酸等を用い
る方法が知られていた。In order to prevent such an increase in adult diseases of the circulatory system, it is necessary to improve the balance of blood lipids such as hyperlipidemia, which causes arteriosclerosis. Further, a method of ingesting a polyunsaturated fatty acid such as linoleic acid and a method of using chlorofibrate or nicotinic acid have been known.
【0004】しかしながら、多価不飽和脂肪酸の摂取は
長期連用が必要な上、過剰摂取に問題があり、クロロフ
ィブレートは筋けいれん等の副作用があり、またニコチ
ン酸にも全身紅潮や胃腸障害等の副作用が有るといった
問題があった。However, ingestion of polyunsaturated fatty acids requires long-term continuous use, and there is a problem of excessive intake, chlorofibrate has side effects such as muscle cramps, and nicotinic acid also causes systemic flushing and gastrointestinal disorders. There was a problem that there were side effects.
【0005】[0005]
【発明が解決しようとする課題】従って、本発明は血中
脂質量のバランスを改善する作用を有し、動脈硬化を抑
制する効果に優れ、且つ、安全性の高い動脈硬化抑制剤
と、これを含む食品又は循環器疾患治療用の医薬組成物
を提供することを目的とする。Accordingly, the present invention provides an arteriosclerosis inhibitor which has an effect of improving the balance of blood lipid levels, is excellent in the effect of suppressing arteriosclerosis, and is highly safe. An object of the present invention is to provide a food containing or a pharmaceutical composition for treating cardiovascular disease.
【0006】[0006]
【課題を解決するための手段】上記実状に鑑み、本発明
者らは、古来より用いられてきており、その使用につい
て、安全であると思われる、漢方生薬を選択し、その抽
出物を、動脈硬化抑制作用を指標として広くスクリーニ
ングした結果、甘草の抽出物に優れた動脈硬化抑制作用
が有るのを見いだし発明を完成させた。In view of the above situation, the present inventors have selected a Chinese herbal medicine that has been used since ancient times and is considered to be safe for its use, and extract its extract. As a result of extensive screening using the arteriosclerosis-inhibiting effect as an index, the inventors have found that the licorice extract has an excellent arteriosclerosis-inhibiting effect and completed the invention.
【0007】従って、本発明は甘草の抽出物からなる動
脈硬化抑制剤に関する。Accordingly, the present invention relates to an arteriosclerosis inhibitor comprising an extract of licorice.
【0008】また、本発明は上記動脈硬化抑制剤を含有
する食品に関する。The present invention also relates to a food containing the above arteriosclerosis inhibitor.
【0009】更に、本発明は上記動脈硬化抑制剤を含有
する循環器疾患治療用の医薬組成物に関する。Furthermore, the present invention relates to a pharmaceutical composition for treating cardiovascular disease, which comprises the above arteriosclerosis inhibitor.
【0010】ところで、本発明で用いる甘草であるが、
これは豆科グリキリザ属の植物の総称で、洋甘草(G.gl
abra L.)、ナンキンカンゾウ(G.glabra L.var glandu
rifera Regel et Herder)、ウラルカンゾウ(G.uralen
sis Fisch.et DC)、シナカンゾウ(G.echinata L.)、
イヌカンゾウ(G.pallidiflora Maxim)、脹果甘草(G.
infrata BAT)などを指し、このものは漢方生薬として
古くから、中国でも、又、日本に於いても広く用いられ
てきた。その漢方に於ける薬効は鎮痛、解熱、鎮咳等で
あり、血中脂質のバランスの改善や動脈硬化抑制作用に
ついては全く知られていなかった。By the way, the licorice used in the present invention,
This is a general term for plants of the genus Glycyriza, which is a licorice (G.gl.
abra L.), peanut elephant (G.glabra L.var glandu
rifera Regel et Herder), Uralkanzo (G.uralen)
sis Fisch.et DC), Chinese elephant (G.echinata L.),
Dog Lizard (G. pallidiflora Maxim), Licorice licorice (G.
infrata BAT), which has been widely used as a Chinese herbal medicine since ancient times in China as well as in Japan. The medicinal effects in the Kampo medicine are analgesia, antipyretic, antitussive, etc., and nothing was known about the improvement of blood lipid balance and the effect of suppressing arteriosclerosis.
【0011】上記甘草は、血中脂質量のバランスを改善
する作用を有する物質を含んでおり、粉砕した全草を用
いることも可能であるが、抽出により前記成分を含む抽
出物を取り出して、本発明の動脈硬化抑制剤の有効成分
として用いることが好ましい。又、用いる植物の部位と
しては全草でも可能であるが、薬効成分の豊富な根や根
茎が好ましい。本発明に於いて抽出物とは、このような
粉砕物及び抽出物、更に後述する分画物、又はこれらの
濃縮物から選ばれる1種または2種以上を言う。The above licorice contains a substance having an action of improving the balance of blood lipid level, and it is also possible to use crushed whole plants, but an extract containing the above components is taken out by extraction, It is preferably used as an active ingredient of the arteriosclerosis inhibitor of the present invention. Although the whole plant can be used as the plant part to be used, roots and rhizomes rich in medicinal components are preferable. In the present invention, the extract refers to one or more selected from such pulverized products and extracts, the fractions described below, or concentrates thereof.
【0012】甘草の抽出処理は、連続式、バッチ式等の
方法で、常法により冷浸または温浸にて任意の時間行
う。例えば、甘草の根及び根茎を乾燥した後、細切し、
抽出溶媒に、室温で1〜3日間、または抽出溶媒の沸騰
温度で1〜5時間浸漬すれば良い。この時、用いる抽出
溶媒としては、水及びアルコール類、アセトン類等の極
性有機溶媒が良く、これらを単独で用いても2種以上を
混合して用いても良い。その後、必要に応じて不溶物を
ろ過により除去したり、減圧または限外ろ過により濃縮
し、溶媒を乾固させても良い。好ましいものは、温湯抽
出したものをろ過した後凍結乾燥したものであり、この
ものは褐色の吸湿性を有するアモルファスである。The extraction process of licorice is carried out by a continuous method, a batch method or the like by a conventional method by cold soaking or hot soaking for an arbitrary time. For example, licorice roots and rhizomes are dried and then chopped,
It may be immersed in the extraction solvent at room temperature for 1 to 3 days or at the boiling temperature of the extraction solvent for 1 to 5 hours. At this time, as the extraction solvent used, water and polar organic solvents such as alcohols and acetones are preferable, and these may be used alone or in combination of two or more kinds. Then, if necessary, the insoluble matter may be removed by filtration, or the solvent may be dried and solidified by concentration under reduced pressure or ultrafiltration. A preferred one is a hot water extract which is filtered and then freeze-dried, which is a brown hygroscopic amorphous material.
【0013】かくして得られた抽出物を製剤化に用いて
も良いが、更にこの抽出物のうち血中脂質量のバランス
を改善する作用を有する成分を高濃度に含有する分画物
を使用しても良い。分画物を得るためには、上記抽出物
から求める作用の少ない極性が著しく高い部分を除去す
るのが好ましく、その方法としては、液液抽出法、吸着
カラムクロマトグラフィー法、分配カラムクロマトグラ
フィー法、GPCカラムクロマトグラフィー法等が例示
できる。このうち、多孔性スチレンージビニルベンゼン
コポリマーを担体として用いた分配カラムクロマトグラ
フィー法が最も手軽で好ましい。The extract thus obtained may be used for formulation, but a fraction containing a high concentration of a component having an action of improving the balance of blood lipid content in the extract is used. May be. In order to obtain the fractionated product, it is preferable to remove a portion of the above-mentioned extract, which has a very low effect and is extremely high in polarity, and the method includes a liquid-liquid extraction method, an adsorption column chromatography method, and a partition column chromatography method. , GPC column chromatography method and the like. Of these, the partition column chromatography method using a porous styrene-divinylbenzene copolymer as a carrier is the easiest and most preferable.
【0014】多孔性スチレンージビニルベンゼンコポリ
マーを用いて分画を得るには、例えば次のように行えば
良い。即ち、アンバーライトXADー2(オルガノ
(株)製)に上記抽出物を精製水に溶かしたものを通
し、精製水で充分洗浄した後、アルコール類等の極性有
機溶媒で溶出させれば良い。また、バッチ法で行うこと
もできるし、予め、ノルマルヘキサンや石油エーテルで
脱脂処理を行っておいても良い。To obtain a fraction using the porous styrene-divinylbenzene copolymer, for example, the following procedure may be carried out. That is, Amberlite XAD-2 (manufactured by Organo Co., Ltd.) is passed through a solution prepared by dissolving the above extract in purified water, thoroughly washed with purified water, and then eluted with a polar organic solvent such as alcohols. Further, it may be carried out by a batch method, or may be subjected to a degreasing treatment with normal hexane or petroleum ether in advance.
【0015】かくして得られた抽出物及び分画物はとも
に動脈硬化抑制剤として用いることができる。この動脈
硬化抑制剤は、そのまま製剤とすることもできるし、各
種基剤に配合して製剤としても良い。Both the extract and the fraction thus obtained can be used as an arteriosclerosis inhibitor. This arteriosclerosis inhibitor may be directly prepared as a preparation, or may be mixed with various bases to prepare a preparation.
【0016】配合量や基剤の種類は特に限定されるもの
ではなく、剤形に合わせて、適宜、設定すれば良く、例
えば、医薬品としては、錠剤、散剤、顆粒剤、カプセル
剤、坐剤、注射剤、液剤等が例示でき、これらは増量
剤、賦形剤、滑沢剤、崩壊剤、結合剤、矯味矯臭剤等と
共に通常の方法に従って剤形化すれば良い。The compounding amount and the kind of the base are not particularly limited, and may be appropriately set according to the dosage form. For example, the medicines are tablets, powders, granules, capsules and suppositories. , Injections, liquids and the like, and these may be formed into a dosage form by a conventional method together with a filler, an excipient, a lubricant, a disintegrant, a binder, a flavoring agent and the like.
【0017】又、食品としては、一般食品として、種々
の食品原料に抽出物の所要量を加え、通常の製造方法に
より加工することにより、また、健康食品、機能性食品
として植物や抽出物、分画物をそのまま、或いは食べ易
い状態にして使用することができる。As a food, as a general food, a required amount of the extract is added to various food raw materials and processed by a usual production method, and a plant or an extract is added as a health food or a functional food. The fractionated product can be used as it is or in a state in which it is easy to eat.
【0018】これらの組成物に於ける、上記動脈硬化抑
制剤の1日あたりの投与量は、症状、身長、体重、年齢
等により異なるが、成人1人あたり1〜2000mg/
Kg、好ましくは3〜100mg/Kgを1回ないし数
回に分けて投与するのがよい。The daily dose of the above-mentioned arteriosclerosis inhibitor in these compositions varies depending on the symptoms, height, weight, age, etc., but is 1 to 2000 mg / adult per adult.
It is advisable to administer Kg, preferably 3 to 100 mg / Kg, once to several times.
【0019】また、本発明の動脈硬化抑制剤の安全性
は、甘草が古来より広く漢方生薬として用いられてきた
実績より、優れているのは明白である。Further, the safety of the arteriosclerosis inhibitor of the present invention is clearly superior to the fact that licorice has been widely used as a herbal medicine since ancient times.
【0020】[0020]
【実施例】以下に、実施例を挙げて更に詳しく本発明に
ついて説明するが、本発明がこれら実施例に限定を受け
ないことは言うまでもない。The present invention will be described in more detail below with reference to examples, but it goes without saying that the present invention is not limited to these examples.
【0021】実施例1. 製造例1.洋甘草の根および根茎を5〜10mmの長さ
に細切したもの100gに、精製水1000mlを加え
て105℃にて3時間還流して、抽出した。冷却後、ろ
過してろ液を取り、減圧濃縮後凍結乾燥し21.9グラ
ムの動脈硬化抑制剤を褐色アモルファスとして得た。Example 1. Production Example 1. To 100 g of roots and rhizomes of Western licorice finely chopped to a length of 5 to 10 mm, 1000 ml of purified water was added, and the mixture was refluxed at 105 ° C. for 3 hours for extraction. After cooling, the filtrate was collected by filtration, concentrated under reduced pressure and freeze-dried to obtain 21.9 g of an arteriosclerosis inhibitor as a brown amorphous substance.
【0022】実施例2. 製造例2.製造例1の動脈硬化抑制剤6gを30mlの
精製水に溶解させ、アンバーライトXADー2を充填し
たカラムに通し、更に500mlの精製水を流し洗浄し
た。これに99.5%エタノール500mlで溶出さ
せ、減圧濃縮して2.0gの動脈硬化抑制剤を得た。Example 2. Production example 2. 6 g of the arteriosclerosis inhibitor of Production Example 1 was dissolved in 30 ml of purified water, passed through a column packed with Amberlite XAD-2, and further washed with 500 ml of purified water. This was eluted with 500 ml of 99.5% ethanol and concentrated under reduced pressure to obtain 2.0 g of an arteriosclerosis inhibitor.
【0023】実施例3. 製造例3.ウラルカンゾウの根及び根茎を5〜10mm
の長さに細切したもの100gに精製水1000mlを
加えて105℃にて3時間還流して、抽出した。冷却
後、ろ過してろ液を取り、減圧濃縮後凍結乾燥して1
7.8gの動脈硬化抑制剤を褐色アモルファスとして得
た。Example 3. Production example 3. 5-10 mm roots and rhizomes of Urals
1000 ml of purified water was added to 100 g of the shredded product, and the mixture was refluxed at 105 ° C. for 3 hours for extraction. After cooling, it is filtered and the filtrate is taken, concentrated under reduced pressure and freeze-dried to
7.8 g of arteriosclerosis inhibitor was obtained as a brown amorphous.
【0024】実施例4. 製造例4.ナンキンカンゾウの根及び根茎を5〜10m
mの長さに細切したもの100gに精製水500mlと
エタノール500mlを加えて105℃で3時間還流し
て抽出した。冷却後、ろ過してろ液を取り、減圧濃縮後
凍結乾燥して18.4gの動脈硬化抑制剤を得た。Example 4. Production Example 4. 5-10 m roots and rhizomes of quince liquorice
Purified water (500 ml) and ethanol (500 ml) were added to 100 g of finely chopped pieces, and the mixture was refluxed at 105 ° C. for 3 hours for extraction. After cooling, filtration was performed to obtain a filtrate, which was concentrated under reduced pressure and freeze-dried to obtain 18.4 g of an arteriosclerosis inhibitor.
【0025】実施例5. 急性毒性毒性試験 体重15〜25gのddy系マウス1群10匹を用いて
経口投与での急性毒性試験を行った。試料は実施例1〜
4の動脈硬化抑制剤を用いた。それぞれの試料を30%
生理食塩水溶液にし、12g/Kg経口投与し、72時
間後に生死の判定を行った。何れの群に於いても死亡例
を認めなかった。これより本発明の動脈硬化抑制剤の安
全性が高いことが明らかである。Example 5. Acute toxicity and toxicity test An acute toxicity test by oral administration was carried out using 1 group of 10 ddy mice each having a body weight of 15 to 25 g. Samples are from Example 1
No. 4 arteriosclerosis inhibitor was used. 30% for each sample
It was made into a physiological saline solution and orally administered at 12 g / Kg, and after 72 hours, life or death was determined. No deaths were observed in any of the groups. From this, it is clear that the arteriosclerosis inhibitor of the present invention is highly safe.
【0026】実施例6. 動脈硬化抑制作用の評価1 実施例1、3、4の動脈硬化抑制剤について動脈硬化抑
制効果に付いて、評価を行った。即ち、1群10匹の5
週齢ICRマウスを日本クレア製CEー2(80%)及
びセルロースパウダー(20%)の混合固形飼料と水を
自由摂取させて4週間予飼育した。その後、ブランク群
はそのまま混合固形飼料と水を、コントロール群、実施
例1投与群、実施例3投与群、実施例4投与群はCEー
2(80%)及びラード(20%)の高脂肪混合固形飼
料と水を自由摂取させながら、同時にコントロール群と
ブランク群には1重量%カルボキシメチルセルロースナ
トリウム水溶液を、実施例1投与群、実施例3投与群、
実施例4投与群には、それぞれ、実施例1、3、4の動
脈硬化抑制剤を10重量%含有する1重量%カルボキシ
メチルセルロースナトリウム水溶液を0.5ml/匹/
1日の投与量で2週間経口投与した。投与終了後、すべ
てのマウスを16時間絶食させ、採血を行った。得られ
た血液より、常法により血清を分離し、酵素法により総
コレステロール量を、ヘパリンーMn沈澱酵素法により
HDLコレステロール量を測定した。総コレステロール
量よりHDLコレステロール量を減じ、これをHDLコ
レステロール量で除した値を動脈硬化指数とし、この値
を用いて動脈硬化抑制作用の指標とした。結果を表1に
示す。なお、ここで*は5%未満の危険率で、**は1
%未満の危険率でコントロール群と有意差が有ったこと
を示す。これより、本発明の動脈硬化抑制剤は優れた動
脈硬化抑制作用を有することが判る。Example 6. Evaluation 1 of Arteriosclerosis Inhibitory Action The arteriosclerosis inhibitory effects of the arteriosclerosis inhibitor of Examples 1, 3 and 4 were evaluated. That is, 5 per group of 10
A week-old ICR mouse was preliminarily bred for 4 weeks by freely ingesting a mixed solid feed of CE-2 (80%) manufactured by CLEA Japan and cellulose powder (20%) and water. After that, the blank group was mixed with the mixed solid feed and water as it was, and the control group, the Example 1 administration group, the Example 3 administration group, and the Example 4 administration group were CE-2 (80%) and lard (20%) high fat. While freely ingesting the mixed solid feed and water, a 1% by weight sodium carboxymethylcellulose aqueous solution was simultaneously administered to the control group and the blank group in Example 1 administration group, Example 3 administration group,
In the administration group of Example 4, 0.5 ml / animal of 1% by weight sodium carboxymethylcellulose aqueous solution containing 10% by weight of the arteriosclerosis inhibitor of Examples 1, 3, and 4, respectively.
The daily dose was orally administered for 2 weeks. After the administration, all mice were fasted for 16 hours and blood was collected. Serum was separated from the obtained blood by a conventional method, and the total cholesterol amount was measured by the enzyme method and the HDL cholesterol amount was measured by the heparin-Mn precipitation enzyme method. The value obtained by subtracting the amount of HDL cholesterol from the amount of total cholesterol and dividing this by the amount of HDL cholesterol was used as an arteriosclerosis index, and this value was used as an index of the arteriosclerosis suppressing action. The results are shown in Table 1. Note that * is a risk rate of less than 5%, and ** is 1
It shows that there was a significant difference from the control group at a risk rate of less than%. From this, it is understood that the arteriosclerosis inhibitor of the present invention has an excellent arteriosclerosis inhibitory action.
【0027】[0027]
【表1】 [Table 1]
【0028】実施例7. 動脈硬化抑制作用の評価2 実施例2の動脈硬化抑制剤についても実施例6と同様に
動脈硬化抑制作用について評価を行った。結果を表2に
示す。これより本発明の動脈硬化抑制剤が優れた動脈硬
化抑制作用を有しているのが明らかである。Example 7. Evaluation of Arteriosclerosis Inhibitory Action 2 The arteriosclerosis inhibitory action of the arteriosclerosis inhibitor of Example 2 was evaluated in the same manner as in Example 6. The results are shown in Table 2. From this, it is clear that the arteriosclerosis inhibitor of the present invention has an excellent arteriosclerosis inhibitory action.
【0029】[0029]
【表2】 [Table 2]
【0030】実施例8. キャンディーへの配合例1 下記の(A)成分を150℃で加熱溶解し、120℃に
冷却後、(B)成分を添加、攪はん後均一としたものを
成型し、冷却してキャンディーを得た。 (A) 砂糖 58 水飴 30 (B) クエン酸 1 実施例1の動脈硬化抑制剤 10 香料 1Example 8. Mixing Example 1 for Candy: The following (A) component was heated and dissolved at 150 ° C., cooled to 120 ° C., then the (B) component was added, and after stirring, a uniform product was molded and cooled to give a candy. Obtained. (A) Sugar 58 Syrup 30 (B) Citric Acid 1 Arteriosclerosis Inhibitor 10 of Example 1 Perfume 1
【0031】実施例9. キャンディーへの配合例2 下記の(A)成分を150℃で加熱溶解し、120℃に
冷却後、(B)成分を添加、攪はん後均一としたものを
成型し、冷却してキャンディーを得た。 (A) 砂糖 67 水飴 30 (B) クエン酸 1 実施例2の動脈硬化抑制剤 1 香料 1Example 9. Mixing Example 2 for Candy: The following component (A) is heated and dissolved at 150 ° C., cooled to 120 ° C., the component (B) is added, and after stirring, a uniform product is molded and cooled to give a candy. Obtained. (A) Sugar 67 Syrup 30 (B) Citric acid 1 Arteriosclerosis inhibitor 1 of Example 2 1 Perfume 1
【0032】実施例10. グミへの配合例1.下記の(A)成分を110℃で加熱
溶解し、別途膨潤溶解させた(B)成分を添加し、更に
(C)成分を添加し、型に流し込み、1昼夜放置後型か
らはずしてグミを得た。 (A) 砂糖 40 水飴 45 (B) ゼラチン 8 (C) クエン酸 2 実施例3の動脈硬化抑制剤 5Example 10. Mixing example for gummy 1. The following component (A) is melted by heating at 110 ° C., the component (B) separately swollen and dissolved is added, and the component (C) is further added, poured into a mold and left for one day and night, then removed from the mold to remove gummies. Obtained. (A) Sugar 40 Syrup 45 (B) Gelatin 8 (C) Citric Acid 2 Arteriosclerosis Inhibitor 5 of Example 3
【0033】実施例11. グミへの配合例2.下記の(A)成分を110℃で加熱
溶解し、別途膨潤溶解させた(B)成分を添加し、更に
(C)成分を添加し、型に流し込み、1昼夜放置後型か
らはずしてグミを得た。 (A) 砂糖 40 水飴 45 (B) ゼラチン 8 (C) クエン酸 2 実施例4の動脈硬化抑制剤 5Example 11. Mixing example with gummy 2. The following component (A) is melted by heating at 110 ° C., the component (B) separately swollen and dissolved is added, and the component (C) is further added, poured into a mold and left for one day and night, then removed from the mold to remove gummies. Obtained. (A) Sugar 40 starch syrup 45 (B) Gelatin 8 (C) Citric acid 2 Arteriosclerosis inhibitor 5 of Example 4
【0034】実施例12. カプセル剤 下記の(A)成分を均一に混合攪はんし、これに(B)
成分を加えてニーダーにより充分に混練した。これをカ
プセル充填機によりカプセル化しカプセル剤を作成し
た。 (A) スクワレン 15 リノレン酸トリグリセライド 15 小麦胚芽油 10 精製イワシ油 20 αーdートコフェロール 0.2 (B) 脱脂大豆粉末 39.8 実施例2の動脈硬化抑制剤 10Example 12 Capsule The following component (A) is uniformly mixed and stirred, and then (B)
The ingredients were added and thoroughly kneaded with a kneader. This was encapsulated with a capsule filling machine to prepare a capsule. (A) Squalene 15 Triglyceride Linolenic Acid 15 Wheat Germ Oil 10 Refined Sardine Oil 20 α-d Tocopherol 0.2 (B) Defatted Soybean Powder 39.8 The Atherosclerosis Inhibitor of Example 2 10
【0035】実施例13. 錠剤 下記成分を均一に混合し、流動層造粒法により造粒し、
乾燥させた。これを打錠機で打錠し錠剤を得た。 デキストリン 15 乳糖 5 パラチノース 15 バレイショデンプン 40 ステアリン酸マグネシウム 5 実施例3の動脈硬化抑制剤 20Example 13. Tablet The following ingredients are mixed uniformly and granulated by the fluidized bed granulation method,
Dried. This was tableted with a tableting machine to obtain tablets. Dextrin 15 Lactose 5 Palatinose 15 Potato starch 40 Magnesium stearate 5 Arteriosclerosis inhibitor of Example 3 20
【0036】実施例14. 顆粒剤 下記(A)成分をグラッド造粒機に入れ、(B)成分の
5%水溶液を滴下しながら造粒し、40℃で乾燥させ、
整粒し顆粒剤を得た。 (A) 乳糖 67.5 コーンスターチ 10 実施例4の動脈硬化抑制剤 20 (B) ヒドロキシプロピルセルロース 2.5Example 14 Granules The following component (A) is placed in a glad granulator, and a 5% aqueous solution of component (B) is added dropwise to granulate, followed by drying at 40 ° C.
The particles were sized to obtain granules. (A) Lactose 67.5 Corn starch 10 Arteriosclerosis inhibitor of Example 4 20 (B) Hydroxypropyl cellulose 2.5
【0037】[0037]
【発明の効果】本発明の動脈効果抑制剤は安全性が高い
上に優れた動脈効果抑制作用を有するので、循環器の疾
病の予防と治療にたいへん有益である。INDUSTRIAL APPLICABILITY Since the agent for suppressing arterial effect of the present invention is highly safe and has an excellent effect for suppressing arterial effect, it is very useful for prevention and treatment of diseases of the circulatory system.
Claims (4)
で抽出されたことを特徴とする請求項1又は2記載の動
脈硬化抑制剤。2. The arteriosclerosis inhibitor according to claim 1 or 2, wherein the extract is extracted with water and / or a polar organic solvent.
含有する食品。3. A food containing the arteriosclerosis inhibitor according to claim 1.
含有する循環器疾患治療用の医薬組成物。4. A pharmaceutical composition for treating cardiovascular disease, which comprises the arteriosclerosis inhibitor according to claim 1.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP22798293A JP3204348B2 (en) | 1993-08-20 | 1993-08-20 | Arteriosclerosis inhibitor and food or medicine containing it |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP22798293A JP3204348B2 (en) | 1993-08-20 | 1993-08-20 | Arteriosclerosis inhibitor and food or medicine containing it |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPH0753393A true JPH0753393A (en) | 1995-02-28 |
| JP3204348B2 JP3204348B2 (en) | 2001-09-04 |
Family
ID=16869311
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP22798293A Expired - Fee Related JP3204348B2 (en) | 1993-08-20 | 1993-08-20 | Arteriosclerosis inhibitor and food or medicine containing it |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JP3204348B2 (en) |
Cited By (7)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| KR100385524B1 (en) * | 2000-07-26 | 2003-05-27 | 정태호 | Herb composition for prevention of atherosclerosis |
| KR20040030376A (en) * | 2002-10-02 | 2004-04-09 | 천연제약 주식회사 | Pharmaceutical composition for treatment of thrombosis |
| KR100970826B1 (en) * | 2008-06-30 | 2010-07-16 | 원광대학교산학협력단 | Composition comprising mixed herbal extract for preventing and treating vascular disease |
| US8071141B2 (en) * | 2000-12-12 | 2011-12-06 | Kaneka Corporation | Compositions for preventing or ameliorating multiple risk factor syndromes |
| JP2013035807A (en) * | 2011-08-10 | 2013-02-21 | Rohto Pharmaceutical Co Ltd | Elastic-fiber formation promotor |
| JP2013035808A (en) * | 2011-08-10 | 2013-02-21 | Rohto Pharmaceutical Co Ltd | Ltbp-4 production promotor |
| KR101461588B1 (en) * | 2012-09-26 | 2014-11-19 | 한국 한의학 연구원 | Pharmaceutical composition for preventing or treating arteriosclerosis |
-
1993
- 1993-08-20 JP JP22798293A patent/JP3204348B2/en not_active Expired - Fee Related
Cited By (7)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| KR100385524B1 (en) * | 2000-07-26 | 2003-05-27 | 정태호 | Herb composition for prevention of atherosclerosis |
| US8071141B2 (en) * | 2000-12-12 | 2011-12-06 | Kaneka Corporation | Compositions for preventing or ameliorating multiple risk factor syndromes |
| KR20040030376A (en) * | 2002-10-02 | 2004-04-09 | 천연제약 주식회사 | Pharmaceutical composition for treatment of thrombosis |
| KR100970826B1 (en) * | 2008-06-30 | 2010-07-16 | 원광대학교산학협력단 | Composition comprising mixed herbal extract for preventing and treating vascular disease |
| JP2013035807A (en) * | 2011-08-10 | 2013-02-21 | Rohto Pharmaceutical Co Ltd | Elastic-fiber formation promotor |
| JP2013035808A (en) * | 2011-08-10 | 2013-02-21 | Rohto Pharmaceutical Co Ltd | Ltbp-4 production promotor |
| KR101461588B1 (en) * | 2012-09-26 | 2014-11-19 | 한국 한의학 연구원 | Pharmaceutical composition for preventing or treating arteriosclerosis |
Also Published As
| Publication number | Publication date |
|---|---|
| JP3204348B2 (en) | 2001-09-04 |
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