JP3108675B2 - Lipid metabolism improver - Google Patents
Lipid metabolism improverInfo
- Publication number
- JP3108675B2 JP3108675B2 JP10066928A JP6692898A JP3108675B2 JP 3108675 B2 JP3108675 B2 JP 3108675B2 JP 10066928 A JP10066928 A JP 10066928A JP 6692898 A JP6692898 A JP 6692898A JP 3108675 B2 JP3108675 B2 JP 3108675B2
- Authority
- JP
- Japan
- Prior art keywords
- lipid metabolism
- chitosan
- improving
- borep
- effect
- 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.)
- Expired - Lifetime
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- Fodder In General (AREA)
- Coloring Foods And Improving Nutritive Qualities (AREA)
- Medicines That Contain Protein Lipid Enzymes And Other Medicines (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
Description
【0001】[0001]
【発明の属する技術分野】本発明は食餌脂質吸収阻害、
食後高脂血症改善作用を有する、高脂血症、動脈硬化
症、肥満などの予防・改善効果を期待できる脂質代謝改
善剤に関する。TECHNICAL FIELD The present invention relates to the inhibition of dietary lipid absorption,
The present invention relates to a lipid metabolism-improving agent which has a postprandial hyperlipidemia-ameliorating effect and is expected to have a preventive / ameliorating effect on hyperlipidemia, arteriosclerosis, obesity and the like.
【0002】[0002]
【従来の技術】近年、食生活の向上ないし洋風化に伴っ
て、脂質の摂取量が増加している。国民栄養調査による
と、昭和63年以降は摂取エネルギーに占める脂質エネ
ルギー比率が適正比率の上限(25%)を超えており、
増加の一途を辿っている。なかでも若い世代を中心に、
動物性脂肪の摂取比率の増加が顕著である。このような
恒常的な脂肪の過剰摂取は、肥満や血清脂質の上昇を引
き起こし、それにともなうさまざまな合併症(例えば、
循環器系疾患、特に、冠・脳血管疾患、および、乳ガ
ン、大腸ガンなどのある種のガン等の成人病)の発症の
危険率が高まるなど、国民の健康保持、増進のうえから
社会問題となっている。2. Description of the Related Art In recent years, the intake of lipids has been increasing with the improvement of dietary habits or westernization. According to the National Nutrition Survey, the percentage of lipid energy in the energy intake exceeds the upper limit of the appropriate ratio (25%) since 1988,
It is steadily increasing. Especially, especially for the young generation,
The increase in animal fat intake ratio is remarkable. This constant overdose of fat can lead to obesity and elevated serum lipids, with various complications (eg,
Increase the risk of developing cardiovascular diseases, especially coronary and cerebrovascular diseases and adult diseases such as certain types of cancer such as breast cancer and colorectal cancer). It has become.
【0003】とりわけ、循環器系疾患発症のリスク要因
として従来から血中コレステロール濃度の上昇が挙げら
れており、さらに最近ではコレステロールとは独立した
要因として、血中トリグリセリド濃度も問題視されてい
る(Austin, M. A. Am. J. Epidem. 129,249-259(198
9), Carlson L. A. et al. Acta. Med. Scand. 206,351
-360(1979), Carlson L. A. et al. Acta. Med. Scand.
218,207-211(1985),Castelli, W. P. Am. Heart. J. 1
12,432-437(1986))。[0003] In particular, an increase in blood cholesterol concentration has been conventionally cited as a risk factor for the onset of circulatory diseases, and more recently, a blood triglyceride concentration has been regarded as a problem independent of cholesterol ( Austin, MA Am. J. Epidem. 129,249-259 (198
9), Carlson LA et al. Acta.Med. Scand. 206,351
-360 (1979), Carlson LA et al. Acta.Med. Scand.
218, 207-211 (1985), Castelli, WP Am. Heart.J. 1
12,432-437 (1986)).
【0004】脂肪や糖質を摂取すると一過性に食後高脂
血症が起こるが、過剰に摂取すると、食後高脂血症状態
が長く続く。高脂血症とは、血清コレステロール濃度の
上昇、および血清トリグリセリド濃度の上昇を含むが、
高コレステロール血症は動脈硬化の危険因子であること
がよく知られている。また、恒常的に脂肪を過剰に摂取
する状況では、血中トリグリセリド濃度の持続的な上昇
をきたし、血中トリグリセリド濃度の上昇は、高血圧症
や、虚血性心疾患などの動脈硬化性疾患の発症につなが
る危険性が高いことが指摘されている(中村 治雄、医
学のあゆみ 157,771-775(1991)、高トリグリセリド血
症ハンドブック、石川 俊次、薬の知識39,3-8(198
8))。[0004] Ingestion of fats and carbohydrates temporarily causes postprandial hyperlipidemia, but excessive intake leads to prolonged postprandial hyperlipidemia. Hyperlipidemia includes elevated serum cholesterol levels and elevated serum triglyceride levels,
It is well known that hypercholesterolemia is a risk factor for arteriosclerosis. In addition, in a situation where fat is consumed excessively constantly, the blood triglyceride concentration is continuously increased, and the increase in the blood triglyceride concentration may cause the onset of arteriosclerotic diseases such as hypertension and ischemic heart disease. It has been pointed out that there is a high risk of causing hypertension (Hario Nakamura, History of Medicine 157,771-775 (1991), Handbook of Hypertriglyceridemia, Shunji Ishikawa, Knowledge of Medicine 39,3-8 (198
8)).
【0005】また、脂質の過剰摂取によるエネルギー過
剰は、肥満の原因となり、肥満は循環不全、動脈硬化、
糖尿病などの成人病の発症率を上昇させる。[0005] Excessive energy due to excessive intake of lipids causes obesity, and obesity causes circulatory failure, arteriosclerosis,
Increase the incidence of adult diseases such as diabetes.
【0006】このため、体脂肪除去あるいは食餌脂質の
低下を目的としたアプローチが精力的に行われており、
以下のような方法、薬物が提案されている。まず、脂肪
摂取量の抑制として、食事療法、脂肪代替品、食欲抑制
剤がある。しかし、食事療法は過度な制限食であること
が多く、脂質に富んだ美味な食品が豊富な現代社会にお
いて、長期的に実行するには非常な困難を伴う。また、
脂肪代替品として、様々な商品が開発されているが、自
然なおいしさ、本物の旨さを追求するグルメの時代に代
替品の味で満足することも容易ではない。更に、最近、
脂肪代替品のあるものでは重篤な副作用が発現すること
が注目されている。また、食欲抑制剤として、マジンド
ールやフェンフルラミン等が知られているが、医師のコ
ントロール下でしか投与できず、その副作用も報告され
ている(Hadler A. J. J. Clin.Pharm. 12,453(1972),
Stunkar D. A. et al. Lanset 1,503(1973))。For this reason, approaches aimed at removing body fat or reducing dietary fat have been vigorously conducted.
The following methods and drugs have been proposed. First, there are a diet, a fat substitute, and an appetite suppressant as the suppression of fat intake. However, diets are often overly restricted diets, and in modern societies rich in delicious foods rich in lipids, are extremely difficult to implement in the long term. Also,
Various products have been developed as fat substitutes, but it is not easy to be satisfied with the taste of substitutes in the era of gourmet pursuit of natural taste and authenticity. More recently,
It has been noted that some fat substitutes have severe side effects. In addition, as an appetite suppressant, mazindol and fenfluramine are known, but can be administered only under the control of a physician, and their side effects have been reported (Hadler AJJ Clin. Pharm. 12,453 (1972),
Stunkar DA et al. Lanset 1,503 (1973)).
【0007】これらのような実行困難な方法に代わるア
プローチとして、脂肪などの摂取には制限を加えず、消
化管での脂質の吸収を抑える薬剤(ニコモール、ネオマ
イシン等)や、吸収した栄養物が脂肪として蓄積する事
を阻止するための薬剤(デヒドロエピアンドロステロン
等)も開発されているが、これらの医薬品においては副
作用の発現が不可避である。[0007] As an alternative to these difficult methods, there are drugs (nicomol, neomycin, etc.) that suppress the absorption of lipids in the gastrointestinal tract without limiting the intake of fats and the like, and the absorbed nutrients. Drugs (such as dehydroepiandrosterone) for preventing accumulation as fat have also been developed, but the occurrence of side effects is inevitable in these drugs.
【0008】その他にも、血中リポタンパク質リパーゼ
活性を高めて血中脂質の代謝を促す医薬品であるデキス
トラン硫酸、脂質代謝改善薬であるクロフィブラートや
ブラバスタチン等が現在用いられているが、これらの医
薬品の投与による副作用も懸念されている。[0008] In addition, dextran sulfate, which is a drug that enhances lipoprotein lipase activity in blood to promote the metabolism of blood lipid, and clofibrate and bravastatin, which are lipid metabolism improvers, are currently used. There are also concerns about the side effects of administering pharmaceuticals.
【0009】高コレステロール血症の治療においては、
コレステロールの生合成を抑えるような薬剤が知られて
いるが、これらの薬物の多くは副作用を伴う。In the treatment of hypercholesterolemia,
Drugs that suppress cholesterol biosynthesis are known, but many of these drugs have side effects.
【0010】そこで、上記の医薬品に対して、副作用の
発現が少ないと考えられる食品素材の開発が期待され
る。食品素材では、種々の食物繊維が消化管内でのコレ
ステロールあるいは胆汁酸の吸収に干渉し、血中コレス
テロール濃度を低下させる事が知られている。有効な食
物繊維としては、ペクチン、グアーガム、コンニャクマ
ンナン、海藻多糖類、キトサン等が挙げられる。[0010] Therefore, development of a food material which is considered to have few side effects with respect to the above-mentioned drugs is expected. In food materials, it is known that various dietary fibers interfere with the absorption of cholesterol or bile acids in the digestive tract and lower blood cholesterol levels. Effective dietary fibers include pectin, guar gum, konjac mannan, seaweed polysaccharides, chitosan and the like.
【0011】近年、キトサンが、他の食物繊維と比較し
て、脂質消化吸収阻害作用において格別優れていること
が動物実験によって明らかとなった。例えば、ラットの
飼料中に5%程度キトサンを添加して飼育した際にはみ
かけの脂肪吸収率の抑制はおよそ50%にも及ぶと報告
されている(金内 理、化学と生物 34,553-557(199
6))。しかしながら、この摂取量を脂肪摂取量あたりで
ヒトに換算すると1日量として15gにもなり、その多
量摂取の結果、強い凝集力によって便秘になるなど、副
作用が現れる可能性が指摘されている。多くの場合、キ
トサン1日最大摂取量は2g以下に設定されている。[0011] In recent years, animal experiments have revealed that chitosan is particularly superior in inhibiting lipid digestion and absorption as compared with other dietary fibers. For example, it has been reported that the suppression of apparent fat absorption reaches as much as 50% when rats are fed with about 5% chitosan added to the diet (Kinari, Chemistry and Biology 34,553-557). (199
6)). However, it has been pointed out that when this intake is converted into humans per fat intake, the daily intake is as much as 15 g, and as a result of the large intake, side effects such as constipation due to strong cohesive strength may occur. In most cases, the maximum daily intake of chitosan is set at 2 g or less.
【0012】さらに、キトサンは消化管における脂肪の
吸収を抑制すると同時に、脂溶性ビタミンの吸収に悪影
響を及ぼす可能性がある。実際、キトサン摂取によって
体内のビタミンA,E血中濃度が減少するという報告が
なされている(金内 理、前出)。ビタミンEには、動
脈硬化を予防する効果があることから、このようなビタ
ミン吸収阻害作用はキトサンに固有の問題点であると考
えられる。Furthermore, chitosan may inhibit fat absorption in the gastrointestinal tract and adversely affect fat-soluble vitamin absorption. In fact, it has been reported that ingestion of chitosan lowers the blood levels of vitamin A and E in the body (Kinari, supra). Since vitamin E has an effect of preventing arteriosclerosis, it is considered that such a vitamin absorption inhibitory action is a problem inherent to chitosan.
【0013】キトサンのコレステロール低下作用は、動
物のみならず、ヒトにおける試験成績が数多く報告され
ており、公知のものである(Sugano, M. et al. Nutr.
Rep.Int., 18, 531-537(1978)、辻 啓介、食品工業 3
6,50-56(1993)、平野 茂博、Food & Food Ingredients
Journal of Japan 159, 65-71(1994)、次田 隆志ら、
月刊フードケミカル45-50(1995)、金内 理、前出)。
しかし、キトサンはヒトに対しては有意に血中コレステ
ロール濃度を減少させるが、血中トリグリセリド値に関
する有意な抑制効果はないという報告もなされている
(辻 啓介、前出、次田ら、前出)。[0013] The cholesterol-lowering effect of chitosan has been reported in many test results not only in animals but also in humans, and is known (Sugano, M. et al. Nutr.
Rep. Int., 18, 531-537 (1978), Keisuke Tsuji, Food Industry 3
6,50-56 (1993), Shigehiro Hirano, Food & Food Ingredients
Journal of Japan 159, 65-71 (1994), Takashi Nishida et al.
Monthly Food Chemical 45-50 (1995), Osamu Kanauchi, supra).
However, it has been reported that chitosan significantly reduces blood cholesterol levels in humans, but has no significant inhibitory effect on blood triglyceride levels (Keiji Tsuji, supra, Nishida et al., Supra). ).
【0014】上記のように、キトサンは消化管における
吸収阻害作用に基づくと考えられる血清コレステロール
濃度上昇抑制物質として優れた食品素材であるが、多量
摂取による副作用等の問題点がある。As described above, chitosan is an excellent food material as a substance that suppresses a rise in serum cholesterol concentration which is considered to be based on the absorption inhibitory action in the digestive tract, but has problems such as side effects due to large intake.
【0015】他方、以下BOREPと称する、「タンパ
ク質又はタンパク質含有物をプロテアーゼ又は酸で加水
分解して製造され、平均ペプチド鎖長が3〜4である脂
質代謝改善作用を有するタンパク質水解物」は、脂肪摂
取による血清トリグリセリド濃度の上昇を顕著に抑制す
る作用を有することが明らかにされている(特公平5-87
052(WO89/06970,US08/608,045))。On the other hand, "a protein hydrolyzate produced by hydrolyzing a protein or a protein-containing substance with a protease or acid and having an average peptide chain length of 3 to 4 and having an effect of improving lipid metabolism," hereinafter referred to as BOREP, It has been shown to have the effect of significantly suppressing the increase in serum triglyceride concentration due to fat intake (Japanese Patent Publication No. 5-87
052 (WO89 / 06970, US08 / 608,045)).
【0016】BOREPの作用としては、膵リパーゼの
活性を抑えることによる消化管における脂質の吸収阻
害、リポタンパク質リパーゼの活性化によるキロミクロ
ン中のトリグリセリドの代謝促進、肝臓での脂肪酸のβ
酸化促進、繊維芽細胞から脂肪前駆細胞、脂肪前駆細胞
から脂肪細胞への変異の抑制、等が確認されており、消
化管での吸収阻害だけでなく、いったん消化吸収された
脂質の代謝を促進するという複数の機構により、血中ト
リグリセリド濃度を低下させると考えられる。The effects of BOREP include inhibition of lipid absorption in the gastrointestinal tract by suppressing the activity of pancreatic lipase, promotion of metabolism of triglyceride in kilomicrons by activation of lipoprotein lipase, and β-
Acceleration of oxidation, suppression of mutation from fibroblasts to preadipocytes, and preadipocytes to adipocytes, etc. have been confirmed, not only inhibiting absorption in the gastrointestinal tract, but also promoting metabolism of lipids once digested and absorbed. It is believed that multiple mechanisms of reducing blood triglyceride levels.
【0017】また、BOREPには、前述のキトサンに
みられる副作用(過剰摂取による副作用、脂溶性ビタミ
ン吸収阻害)はみられない。しかし、BOREPはキト
サンほどの顕著な血中コレステロール上昇抑制作用を示
さないという問題点がある。In addition, BOREP has no side effects (side effects due to excessive intake, inhibition of fat-soluble vitamin absorption) observed in chitosan. However, BOREP has a problem that it does not show a remarkable inhibitory effect on blood cholesterol rise as much as chitosan.
【0018】[0018]
【発明が解決しようとする課題】本発明は、脂質の消化
吸収を阻害するとともに、いったん吸収された脂質の代
謝を改善することによって、上記のような問題点を解決
し、恒常的な脂肪の過剰摂取と因果関係の強い、肥満並
びに高脂血症や動脈硬化症などの生活習慣病の予防効果
および改善効果を有する脂質代謝改善剤を提供すること
を目的とする。DISCLOSURE OF THE INVENTION The present invention solves the above problems by inhibiting the digestion and absorption of lipids and improving the metabolism of the lipids once absorbed. An object of the present invention is to provide a lipid metabolism-improving agent having a prophylactic and ameliorating effect on obesity and lifestyle-related diseases such as hyperlipidemia and arteriosclerosis, which have a strong causal relationship with excessive intake.
【0019】[0019]
【課題を解決するための手段】本発明者らは、上記した
ような事情に鑑み、タンパク質又はタンパク質含有物を
プロテアーゼ又は酸で加水分解して製造され、平均ペプ
チド鎖長が3〜4である脂質代謝改善作用を有するタン
パク質水解物(BOREPと称する)と、キトサンとを
実際に初めて混合して用いることにより、その配合剤
に、血中トリグリセリド濃度上昇抑制作用および血中コ
レステロール濃度上昇抑制作用において、予想外にも相
乗効果を見出し、さらに、投与量などにおいて、それぞ
れの成分の単一投与時にみられる問題点を補い、各成分
の単一投与時には見られなかった格別顕著な効果が発揮
されることを見出し、これらに基づいて本発明を完成し
た。特に当該混合物を用いることによって、キトサンの
摂取量を大幅に減じることができる。Means for Solving the Problems In view of the circumstances described above, the present inventors have produced a protein or a protein-containing substance by hydrolysis with a protease or an acid, and have an average peptide chain length of 3 to 4. By actually mixing and using a protein hydrolyzate (referred to as BOREP) having a lipid metabolism improving effect and chitosan for the first time, the combination drug has an effect of suppressing a blood triglyceride concentration increase and a blood cholesterol concentration increase. , Unexpectedly found a synergistic effect, further supplemented the problems seen in the single administration of each component in the dosage, etc., exhibited exceptional remarkable effects that were not seen in the single administration of each component The present invention was completed based on these. In particular, by using the mixture, the intake of chitosan can be significantly reduced.
【0020】即ち、本発明による脂質代謝改善剤は、B
OREPとキトサンとの混合物を有効成分として含有す
ることを特徴とする。That is, the lipid metabolism improving agent according to the present invention comprises B
It is characterized by containing a mixture of OREP and chitosan as an active ingredient.
【0021】本発明で使用するBOREPは、例えば特
公平5-87052(国際公開番号WO89/06970)および国際公
開番号WO97/00890などに開示され、これらの公報の開示
に記載の方法又はそれに準ずる方法に従って製造するこ
とができる。また、本発明で使用するキトサンはそれ自
身公知であり、例えば、キチン・キトサン研究会編「最
後のバイオマス キチン、キトサン 1988年刊」に
詳細に記載されている。本発明でも、市販のものから適
当なものを選んで使用することができる。The BOREP used in the present invention is disclosed in, for example, Japanese Patent Publication No. 5-87052 (International Publication No. WO89 / 06970) and International Publication No. WO97 / 00890, and the method described in these publications or a method analogous thereto. It can be manufactured according to The chitosan used in the present invention is known per se, and is described in detail, for example, in Chitin-Chitosan Research Society, "Last Biomass Chitin, Chitosan, 1988". Also in the present invention, an appropriate one can be selected from commercially available ones.
【0022】BOREPとキトサンの配合重量比は、自
由に設定できるが、後述の実施例に示すように、好まし
くは4:1〜2:3であり、さらに好ましくは3:2程
度である。この配合重量比において高い相乗効果が得ら
れる。The blending weight ratio of BOREP and chitosan can be freely set, but is preferably from 4: 1 to 2: 3, more preferably about 3: 2, as shown in the examples described later. A high synergistic effect can be obtained at this compounding weight ratio.
【0023】本発明による脂質代謝改善剤は、動物
(例、ヒト、ウサギ、マウス等)に対して食餌脂質吸収
阻害作用、及び、食後高脂血症改善作用に基づくと考え
られる脂質代謝改善作用を示し、高脂血症(高トリグリ
セリド血症、高コレステロール血症)、動脈硬化症(ア
テローム性動脈硬化症、脳動脈硬化症、冠動脈硬化症、
末梢動脈硬化症等)高血圧症、肥満症の、予防・改善剤
として有用である。本発明による前記改善剤は、肥満
症、高脂血症、等の高血圧症を合併症とする疾患の予防
または改善に顕著な効果を奏し、とりわけ、高血圧症を
合併症とする動脈硬化症の予防・改善に好ましく用いら
れる。The agent for improving lipid metabolism according to the present invention has an effect of inhibiting dietary lipid absorption in animals (eg, humans, rabbits, mice, etc.) and an effect of improving lipid metabolism which is considered to be based on an effect of improving postprandial hyperlipidemia. Indicates hyperlipidemia (hypertriglyceridemia, hypercholesterolemia), arteriosclerosis (atherosclerosis, cerebral atherosclerosis, coronary atherosclerosis,
It is useful as a prophylactic / ameliorating agent for hypertension and obesity. The ameliorating agent according to the present invention has a remarkable effect in preventing or ameliorating diseases associated with hypertension, such as obesity, hyperlipidemia, and the like. It is preferably used for prevention and improvement.
【0024】本発明による脂質代謝改善剤は、それ自体
の標品(BOREP原体とキトサン原体の混合物)ある
いは適宜の担体、賦形剤、希釈剤等と混合し、カプセル
剤、錠剤、粉末、顆粒等の固形組成物として、経口的に
安全に投与することができる。これらの組成物は製剤化
工程において一般に用いる公知の方法に従って製剤化す
ることができる。The lipid metabolism-improving agent according to the present invention can be used as a preparation itself (mixture of a BOREP substance and a chitosan substance) or mixed with an appropriate carrier, excipient, diluent, etc. to obtain capsules, tablets, powders and the like. And can be safely administered orally as a solid composition such as granules. These compositions can be formulated according to known methods generally used in the formulation process.
【0025】個々の成分の1日投与量は、例えば約45
0〜900mgの範囲のBOREPと、例えば約300
〜600mgの範囲のキトサンを有効に組み合わせるこ
とが出来る。当然ながら、これらの用量範囲は1日投与
量を分割するために必要な単位ベースで調節できる。好
ましくは、以下の実施例に記載するような錠剤を1日6
〜12錠、最も好ましくは1日8錠(BOREP600
mg、キトサン400mg)投与される。The daily dosage of the individual components may be, for example, about 45
BOREP in the range of 0-900 mg, for example, about 300
Chitosan in the range of 600600 mg can be effectively combined. Of course, these dose ranges can be adjusted on a unit basis necessary to divide up the daily dose. Preferably, tablets as described in the Examples below are administered 6 times a day.
~ 12 tablets, most preferably 8 tablets daily (BOREP 600
mg, chitosan 400 mg).
【0026】本発明による脂質代謝改善剤は以上のよう
な製剤として提供されるばかりでなく、それを飲食品お
よび動物用飼料に含有させた形態として提供される。こ
れらの飲食品および動物用飼料は、脂質代謝改善用の用
途に用いられる。食品としては、健康食品、特定保健用
食品、一般の食品(チョコレート、ケーキ、ハム、ミー
トソース、シチュー、ミルク、プリン、カレー、ハヤシ
等)が挙げられる。これらの食品に本発明による脂質代
謝改善剤を0.1〜50%の割合で混合し、前記改善剤
が1日あたり750mg〜1200mgとなる範囲で投
与するのが好ましい。動物用飼料においては、前記改善
剤を0.05%〜5%の範囲で含有させることが好まし
い。本発明による脂質代謝改善剤を配合した動物用飼料
は、動物の高脂肪化を防ぐことにより、畜産、水産分野
における動物の肉質の改善に有用である。The lipid metabolism-improving agent according to the present invention is provided not only as a preparation as described above, but also as a form containing it in foods and drinks and animal feed. This
These foods and drinks and animal feeds are used to improve lipid metabolism.
Used for purposes. Examples of the food include health foods, foods for specified health use, and general foods (chocolate, cake, ham, meat sauce, stew, milk, pudding, curry, coconut, etc.). It is preferable that the lipid metabolism improving agent according to the present invention is mixed with these foods at a ratio of 0.1 to 50%, and the improving agent is administered in a range of 750 mg to 1200 mg per day. In animal feeds, it is preferable that the improving agent is contained in a range of 0.05% to 5%. The animal feed containing the agent for improving lipid metabolism according to the present invention is useful for improving animal meat quality in the fields of livestock and fisheries by preventing the animal from becoming fat.
【0027】[0027]
【発明の実施の形態】本発明の一成分であるBOREP
の製法は特公 平5-87052に開示されているが、その一
例は次のようである。動物性、植物性、微生物起源など
の任意のタンパク質又はタンパク質含有物を固形分とし
て水に5〜30重量%となるように分散させ、酸または
アルカリによってプロテアーゼの至適pHに調整し、プ
ロテアーゼを一度にまたは逐次的に添加して、20〜7
0℃の温度で3〜48時間、プロテアーゼを反応させて
加水分解する。BEST MODE FOR CARRYING OUT THE INVENTION BOREP which is a component of the present invention
The production method is disclosed in Japanese Patent Publication No. 5-87052, an example of which is as follows. Any protein or protein-containing substance such as animal, vegetable, or microbial sources is dispersed as a solid in water at 5 to 30% by weight, and the protease is adjusted to an optimal pH with an acid or an alkali. Add all at once or sequentially to 20-7
The protease is reacted and hydrolyzed at a temperature of 0 ° C. for 3-48 hours.
【0028】次に、得られたタンパク質分解物を噴霧乾
燥して、または当該タンパク質分解物にカルボキシメチ
ルセルロースあるいはデキストリンといった増量剤を適
量加えて、乾燥、固化することにより、脂質代謝改善効
果を有するタンパク質水解物であるBOREPの固形物
を得ることができる。Next, the obtained protein hydrolyzate is spray-dried, or an appropriate amount of a bulking agent such as carboxymethylcellulose or dextrin is added to the protein hydrolyzate and dried and solidified to obtain a protein having an effect of improving lipid metabolism. BOREP solids, which are hydrolysates, can be obtained.
【0029】BOREPの原材料としては上記のように
任意のタンパク質を用いることができるが、国際公開番
号WO97/00890に記載のようにヘモグロビンやミオグロビ
ン等のグロビンタンパク質が、血中トリグリセリド濃度
の上昇を抑制するという効果を強く奏しうるという点に
おいて特に好ましい。As a raw material of BOREP, any protein can be used as described above. However, as described in International Publication No. WO97 / 00890, globin proteins such as hemoglobin and myoglobin suppress increase in blood triglyceride concentration. This is particularly preferable in that the effect of performing the above can be strongly exerted.
【0030】なお、そのようなグロビンタンパク質の供
給源である動物の種類は特に限定されず、ウシ、ブタ、
ヒツジ、ヒト、ウマ等の血液を広く用いることが出来
る。The kind of animal that is the source of such a globin protein is not particularly limited, and it may be cow, pig,
Blood from sheep, humans, horses, etc. can be used widely.
【0031】また、用いる加水分解酵素としては、例え
ば酸性プロテアーゼ、中性プロテアーゼ又はアルカリ性
プロテアーゼの一種もしくは二種以上を用いることが出
来る。As the hydrolase to be used, for example, one or more of acidic protease, neutral protease and alkaline protease can be used.
【0032】このような、加水分解により得られたBO
REPの有効成分としては、数種のオリゴペプチドが確
認されており、例えば、国際出願番号WO97/00890では、
BOREPの構成成分の中でも、特に、Leu-Val-Val-Ty
r-Pro-Trp-Thr, Val-Thr-Leu, Val-Tyr-Proの3種のペ
プチドが、またWO97/35875では、Val-Val-Tyr-Proが、
いずれも血中トリグリセリド濃度上昇抑制作用において
優れていることが確認されている。The BO obtained by the hydrolysis as described above
As an active ingredient of REP, several oligopeptides have been confirmed. For example, in International Application No. WO97 / 00890,
Among the components of BOREP, in particular, Leu-Val-Val-Ty
Three peptides of r-Pro-Trp-Thr, Val-Thr-Leu and Val-Tyr-Pro, and in WO97 / 35875, Val-Val-Tyr-Pro
All have been confirmed to be excellent in the action of suppressing the increase in blood triglyceride concentration.
【0033】本発明のもう一つの成分であるキトサン
は、前述したように公知の物質であり、例えば、キチン
・キトサン研究会編「最後のバイオマス キチン、キト
サン1988年刊」に詳細に記載されている。本発明で
も、市販のものから適当なものを選んで使用することが
できる。Chitosan, another component of the present invention, is a known substance as described above, and is described in detail, for example, in "The Last Biomass Chitin, Chitosan, 1988" edited by Chitin and Chitosan Research Society. . Also in the present invention, an appropriate one can be selected from commercially available ones.
【0034】[0034]
【実施例】実施例1:血清脂質濃度上昇に対する抑制効
果(マウスを用いた実験)EXAMPLES Example 1: Inhibitory effect on increase in serum lipid concentration (experiment using mice)
【0035】固形飼料(CE−2、日本クレア株式会
社)で予備飼育して順化したICR雄性マウス(6〜7
週齢、33g程度)を無作為に6群(BOREP投与
群、キトサン投与群、および以下、本発明品と称するB
OREPとキトサンの混合物(BOREPとキトサンの
配合比率 4:1,3:1,3:2,2:3)投与群)
に分けて使用した。一夜絶食後、コレステロール5%添
加オリーブ油250mgと、上記の投与物をそれぞれの
群に経口投与し、投与2時間後に、血清トリグリセリド
濃度および血清コレステロール濃度を酵素法により測定
した。測定は和光純薬製の「トリグリセリドE−テス
ト」、「コレステロールE−テスト」を用い、キットに
指示されているプロトコールに従って行った。Adapted ICR male mice (6-7) preliminarily reared on solid feed (CE-2, CLEA Japan)
6 weeks (about 33 g) were randomly selected into 6 groups (BOREP administration group, chitosan administration group, and hereafter referred to as the product of the present invention B)
A mixture of OREP and chitosan (BOREP and chitosan combination ratio 4: 1, 3: 1, 3: 2, 2: 3) administration group)
Used separately. After an overnight fast, 250 mg of olive oil supplemented with 5% cholesterol and the above-mentioned administration were orally administered to each group, and two hours after administration, serum triglyceride concentration and serum cholesterol concentration were measured by an enzyme method. The measurement was performed using "Triglyceride E-test" and "Cholesterol E-test" manufactured by Wako Pure Chemical Industries, Ltd., according to the protocol specified in the kit.
【0036】測定濃度値から、各投与物における血清脂
質濃度上昇抑制作用の50%抑制率(ID50 mg/mouse)
を求めた結果(表中測定値)を以下の表1、表2に示
す。表中の比率(B:C)は本発明品におけるBORE
P:キトサンの配合比率を示す。本発明品のID50(表中
(b))はBOREP、キトサン単独のID50測定値に、そ
れぞれの配合比率をかけたものを加えて得られる相加効
果を想定した理論値である。相乗効果は、本発明品の計
算値に対する測定値の百分率で示す。この値が小さい
程、二成分の組み合わせによる相乗効果が大きいことを
意味する。From the measured concentration values, a 50% inhibition rate (ID50 mg / mouse) of the inhibitory effect on the increase in serum lipid concentration in each administered substance.
(Measured values in the table) are shown in Tables 1 and 2 below. The ratio (B: C) in the table is the BORE in the product of the present invention.
P: Indicates the compounding ratio of chitosan. ID50 of the product of the present invention (in the table
(b)) is a theoretical value assuming an additive effect obtained by adding the values obtained by multiplying the measured values of ID50 of BOREP and chitosan alone by their respective mixing ratios. The synergistic effect is expressed as a percentage of the measured value with respect to the calculated value of the product of the present invention. The smaller this value, the greater the synergistic effect of the combination of the two components.
【0037】[0037]
【表1】 [Table 1]
【0038】[0038]
【表2】 [Table 2]
【0039】表1、表2のデータを視覚的に把握、検討
するために、ID50測定値を図1、図2にそれぞれプロッ
トした。BOREPおよびキトサンの単独のID50を結ん
だ図中の直線は、相加効果の計算値(理論値)を連続的
にプロットしたものである。本発明品のID50測定値(図
中開四角で記したプロット)はこの直線よりも原点側に
プロットされ、いずれの配合比率においても相乗効果が
あることが認められた。In order to visually grasp and examine the data in Tables 1 and 2, the measured ID50 values were plotted in FIGS. 1 and 2, respectively. The straight line in the figure connecting the ID50 of BOREP and chitosan alone is a continuous plot of the calculated value (theoretical value) of the additive effect. The measured values of ID50 of the product of the present invention (plots indicated by open squares in the figure) were plotted on the origin side with respect to this straight line, and it was confirmed that there was a synergistic effect at any mixing ratio.
【0040】この実験からBOREPとキトサンを配合
することによって、トリグリセリド濃度上昇およびコレ
ステロール濃度上昇に対する抑制効果に関して、各成分
を単に混合した際に推測される効果に比較して、予想外
に強い相乗効果を発揮することが明らかとなった。According to this experiment, the combination of BOREP and chitosan has an unexpectedly strong synergistic effect on the inhibitory effects on the increase in triglyceride concentration and cholesterol concentration as compared to the effect expected when each component is simply mixed. It became clear that it exhibited.
【0041】実施例2:血清脂質濃度上昇に対する抑制
効果(ウサギを用いた実験)Example 2 Inhibitory Effect on Serum Lipid Concentration Increase (Experiment Using Rabbit)
【0042】固形飼料(CR−1,日本クレア株式会
社)で予備飼育して順化したNZW雄性ウサギ(7週
齢、3〜4kg程度)16匹を無作為に4群(対照群、
BOREP投与群、キトサン投与群、および本発明品
(BOREPとキトサンの配合比率3:2)投与群)に
分けて使用した。Sixteen randomized NZW male rabbits (7 weeks old, about 3 to 4 kg) which had been preliminarily reared on a solid feed (CR-1, Nippon Clea Co., Ltd.) (control group,
They were divided into a BOREP administration group, a chitosan administration group, and a product of the present invention (a BOREP / chitosan combination ratio of 3: 2) administration group.
【0043】対照群はコレステロールを1%添加した飼
料で2週間飼育した。他の3群は前記コレステロール1
%添加飼料に、各投与物をそれぞれ5%添加した配合飼
料で2週間飼育した。この2週間の飼育期間の開始時,
1週間経過時,2週間経過時に耳介静脈から採血(0.
5〜1ml)し、血清トリグリセリド濃度および血清コ
レステロール濃度を酵素法で測定した。測定は和光純薬
製の「トリグリセリドE−テスト」、「コレステロール
E−テスト」を用いて行った。これらの結果を表3およ
び表4に示す。各投与群の対照群に対する効果(表中
a)、および本発明群に対する効果(表中b)を、有意
差検定法(Fisher's PLSD法)によって検討し、危険率P
<0.05の場合の差を有意であると判定した。The control group was bred for 2 weeks on a diet supplemented with 1% cholesterol. The other three groups are the cholesterol 1
The feed was bred for 2 weeks on a feed mixture containing 5% of each of the administered substances. At the beginning of this two week breeding period,
Blood is collected from the auricular vein after 1 week and 2 weeks (0.
5 to 1 ml), and the serum triglyceride concentration and serum cholesterol concentration were measured by an enzyme method. The measurement was performed using "Triglyceride E-test" and "Cholesterol E-test" manufactured by Wako Pure Chemical. The results are shown in Tables 3 and 4. The effect of each administration group on the control group (a in the table) and the effect on the present invention group (b in the table) were examined by a significant difference test method (Fisher's PLSD method).
The difference in the case of <0.05 was determined to be significant.
【0044】[0044]
【表3】 [Table 3]
【0045】[0045]
【表4】 [Table 4]
【0046】対照群と比較して、BOREP、キトサン
および本発明品を投与した群の血清トリグリセリド濃度
および血清コレステロール濃度はともに低下した。BO
REPは、脂肪摂取による血清トリグリセリド濃度上昇
を有意に抑制することが知られていたが、反復摂取によ
って血清トリグリセリド濃度だけでなくコレステロール
濃度に対しても抑制効果を示すことが明かとなった。As compared with the control group, the serum triglyceride concentration and the serum cholesterol concentration of the group to which BOREP, chitosan and the product of the present invention were administered were both reduced. BO
REP was known to significantly suppress the increase in serum triglyceride concentration due to fat ingestion, but it was revealed that repeated ingestion showed an inhibitory effect not only on serum triglyceride concentration but also on cholesterol concentration.
【0047】さらに、飼育2週間後の結果から明らかな
ように、本発明品は、血清トリグリセリドおよび血清コ
レステロール濃度上昇の両方について、配合成分である
BOREPおよびキトサンの単独投与に比べて強い抑制
効果を示した。この結果から本発明品が、BOREP、
キトサン単独投与と比較して、食後高脂血症(高トリグ
リセリド血症、高コレステロール血症)抑制剤として有
用であることが示された。Further, as is clear from the results after 2 weeks of rearing, the product of the present invention has a stronger inhibitory effect on both serum triglyceride and serum cholesterol concentration than the single administration of the combined components BOREP and chitosan. Indicated. From these results, the product of the present invention was found to be BOREP,
It was shown to be useful as an inhibitor of postprandial hyperlipidemia (hypertriglyceridemia, hypercholesterolemia) as compared to chitosan alone.
【0048】実施例3:血清脂質濃度上昇に対する抑制
効果(ヒト試験)Example 3: Inhibitory effect on increase in serum lipid concentration (human test)
【0049】血清トリグリセリドあるいはコレステロー
ル濃度が正常から境界領域のレベルの成人ボランティア
(男子12例、年齢27〜50歳)を対象とした。試験
はヘルシンキ宣言の趣旨に従って行い、被験者は試験に
関する十分な説明を受けたうえで、自らの意志で同意書
に署名した。試験は交叉法で行い、試験間の休止期間は
1週間とした。[0049] Adult volunteers (12 males, ages 27-50 years) with serum triglyceride or cholesterol levels at levels from the normal to the border region were used. The test was conducted in accordance with the Helsinki Declaration, and the subjects signed the consent form at their own volition after receiving sufficient explanation about the test. The test was performed by the crossover method, and the rest period between tests was one week.
【0050】試験方法の概要は以下の通りである。被験
者は前夜から12時間以上絶食し、翌朝9時に鶏卵5個
とバター50gで調理したオムレツを摂食した。食後、
BOREP投与群、キトサン投与群、本発明品(BOR
EPとキトサンの配合比率3:2)投与群はそれぞれの
成分を1g含有する錠剤を摂取した(本発明品投与群に
おいてはBOREP600mgおよびキトサン400m
g)。対照群については上記成分を含有しない錠剤を摂
取した。摂食したオムレツの栄養成分を表5に示す。The outline of the test method is as follows. The subjects fasted for 12 hours or more from the night before, and ate omelets cooked with 5 chicken eggs and 50 g of butter at 9 am the following morning. After eating,
BOREP administration group, chitosan administration group, the product of the present invention (BOR
The administration group ingested a tablet containing 1 g of each component (in the administration group of the present invention, 600 mg of BOREP and 400 m of chitosan).
g). For the control group, tablets not containing the above components were ingested. Table 5 shows the nutritional components of the ingested omelet.
【0051】[0051]
【表5】 [Table 5]
【0052】食事前(0時間)、食後1,2,3,4,
5,6時間に上腕静脈から採血を行い、血清を分離して
トリグリセリド濃度、総コレステロール濃度を酵素法で
測定した。測定は和光純薬製の「トリグリセリドE−テ
スト」、「コレステロールE−テスト」を用いて行っ
た。血清トリグリセリド濃度の経時的変化を図3に、血
清コレステロール濃度の経時的変化を図5に示す。Before meal (0 hour), after meal 1,2,3,4
Blood was collected from the brachial vein at 5 or 6 hours, the serum was separated, and the concentrations of triglyceride and total cholesterol were measured by the enzyme method. The measurement was performed using "Triglyceride E-test" and "Cholesterol E-test" manufactured by Wako Pure Chemical. FIG. 3 shows the change over time in the serum triglyceride concentration, and FIG. 5 shows the change over time in the serum cholesterol concentration.
【0053】図3および図5に示すように、脂肪食を摂
取することによって血清トリグリセリド濃度および血清
コレステロール濃度は上昇し、BOREP、キトサンお
よび本発明品を投与することによって上昇が抑制され
た。図中の*は危険率P<0.05で、**は危険率P
<0.01で、本発明品投与群が、対照群、BOREP
投与群、キトサン投与群のいずれに対しても有意差を示
すことを表す。図3、図5から理解されるように、本発
明品の投与は、BOREP、キトサン単独投与に比較し
て、脂肪負荷後の血清トリグリセリド濃度上昇、および
血清コレステロール濃度上昇を有意に抑制した。As shown in FIG. 3 and FIG. 5, the serum triglyceride concentration and the serum cholesterol concentration were increased by ingesting the fat diet, and the increase was suppressed by administering BOREP, chitosan and the product of the present invention. In the figure, * represents the risk factor P <0.05, and ** represents the risk factor P.
<0.01, the group treated with the product of the present invention was a control group, BOREP
It indicates that there is a significant difference between the administration group and the chitosan administration group. As can be understood from FIGS. 3 and 5, administration of the product of the present invention significantly suppressed increase in serum triglyceride concentration and increase in serum cholesterol concentration after fat load, as compared to administration of BOREP and chitosan alone.
【0054】図4および図6は、それぞれ血清トリグリ
セリド濃度、血清コレステロール濃度に関する、0〜6
時間のAUC(血清中化合物濃度時間曲線下の面積)を
示す。これらのグラフから明らかなように、血清トリグ
リセリド増加量、血清コレステロール増加量の両方につ
いて、本発明品投与による抑制効果は、BOREP、キ
トサン単独投与による抑制効果と比較して強いものであ
った。FIGS. 4 and 6 show the serum triglyceride concentration and serum cholesterol concentration, respectively, of 0-6.
AUC (area under serum compound concentration time curve) of time is shown. As is clear from these graphs, the inhibitory effect of the administration of the product of the present invention was stronger than that of the administration of BOREP or chitosan alone, for both the increase in serum triglyceride and the increase in serum cholesterol.
【0055】実施例4:錠剤の組成Example 4: Composition of tablet
【0056】本発明による脂質代謝改善剤の錠剤組成の
1例を以下に示す。One example of the tablet composition of the lipid metabolism improving agent according to the present invention is shown below.
【0057】BOREP 75mg、キトサン 50m
g、コーンスターチ 10mg、結晶セルロース 20
mg、乳糖 適量、二酸化ケイ素 2mg、ショ糖脂肪
酸エステル 5mg、以上を錠剤とする(錠剤重量 2
15mg)。BOREP 75mg, Chitosan 50m
g, corn starch 10 mg, crystalline cellulose 20
mg, lactose appropriate amount, silicon dioxide 2 mg, sucrose fatty acid ester 5 mg, and more as tablets (tablet weight 2
15 mg).
【0058】以上の諸例から理解されるように、血清ト
リグリセリド濃度上昇抑制に特に有効なBOREPと、
血清コレステロール濃度上昇抑制に特に有効なキトサン
とを組み合わせてなる本発明の脂質代謝改善剤により、
血清トリグリセリド濃度上昇、血清コレステロール濃度
上昇の両方に対して、上記2成分を単用した際の効果に
比較して、予想外の強い効果(相乗効果)が得られた。
本発明の脂質代謝改善剤は、上記成分を単独で使用する
場合の投与量を大幅に減少させることが可能であり、そ
の結果、ヒトに対して無理のない摂取量で効果を発揮
し、特に高脂血症、動脈硬化症等の予防・改善剤として
有用である。As can be understood from the above examples, BOREP, which is particularly effective in suppressing an increase in serum triglyceride concentration,
The lipid metabolism improving agent of the present invention, which is combined with chitosan, which is particularly effective for suppressing a rise in serum cholesterol concentration,
An unexpectedly strong effect (synergistic effect) was obtained for both the increase in serum triglyceride concentration and the increase in serum cholesterol concentration, as compared with the effect of using the above two components alone.
The lipid metabolism-improving agent of the present invention can significantly reduce the dose when the above components are used alone, and as a result, exerts an effect on humans with reasonable intake, especially It is useful as a prophylactic / ameliorating agent for hyperlipidemia, arteriosclerosis and the like.
【図1】 脂肪負荷後の血清トリグリセリド濃度上昇に
対する抑制効果についてのBOREPとキトサンの配合
による相乗効果のグラフ。FIG. 1 is a graph showing the synergistic effect of the combination of BOREP and chitosan on the inhibitory effect on an increase in serum triglyceride concentration after fat loading.
【図2】 脂肪負荷後の血清コレステロール濃度上昇に
対する抑制効果についてのBOREPとキトサンの配合
による相乗効果のグラフ。FIG. 2 is a graph showing the synergistic effect of the combination of BOREP and chitosan on the inhibitory effect on the increase in serum cholesterol concentration after fat loading.
【図3】 脂肪負荷後の血清トリグリセリド濃度に及ぼ
す発明品の効果の経時的検討のグラフ。FIG. 3 is a graph of a time-course study of the effect of the invention on serum triglyceride concentration after fat loading.
【図4】 脂肪負荷後の血清トリグリセリド増加量(A
UC0−6h)に及ぼす発明品の効果のグラフ。FIG. 4. Serum triglyceride increase after fat loading (A
7 is a graph of the effect of the invention on UC0-6h).
【図5】 脂肪負荷後の血清コレステロール濃度に及ぼ
す発明品の効果の経時的検討のグラフ。FIG. 5 is a graph of a time-course study of the effect of the invention product on serum cholesterol concentration after fat loading.
【図6】 脂肪負荷後の血清コレステロール増加量(A
UC0−6h)に及ぼす発明品の効果のグラフ。FIG. 6: Serum cholesterol increase after fat loading (A
7 is a graph of the effect of the invention on UC0-6h).
───────────────────────────────────────────────────── フロントページの続き (51)Int.Cl.7 識別記号 FI A61K 31/722 A61K 31/722 A61P 3/06 A61P 3/06 (72)発明者 福浜 千津子 大阪府池田市古江町180番地 阪急共栄 物産株式会社 薬理研究所内 (72)発明者 藤野 博昭 大阪府池田市古江町180番地 阪急共栄 物産株式会社 薬理研究所内 (56)参考文献 特開 平7−194316(JP,A) 国際公開89/6970(WO,A1) 国際公開97/890(WO,A1) NUTRITION REPORTS INTERNATIONAL,1978, Vol.18,No.9,pp.531−537 月刊フードケミカル、1995−2、第45 −50ページ 食品工業、1993、第36巻、第50−56ペ ージ FOODS AND FOOD IN GREDIENTS JOURNAL OF JAPAN,1994,No.159, pp.65−71 (58)調査した分野(Int.Cl.7,DB名) A61K 38/01 A23K 1/16 A23L 1/30 A23L 1/305 A61K 31/722 A61P 3/06 CA(STN)──────────────────────────────────────────────────続 き Continued on the front page (51) Int.Cl. 7 Identification code FI A61K 31/722 A61K 31/722 A61P 3/06 A61P 3/06 (72) Inventor Chisuko Fukuhama 180 Koecho, Ikeda-shi, Osaka Hankyu Kyoei Bussan Co., Ltd. Pharmaceutical Research Laboratories (72) Inventor Hiroaki Fujino 180 Kouecho, Ikeda-shi, Osaka Hankyu Kyoei Bussan Co., Ltd. Pharmacological Research Laboratories (56) References JP-A 7-194316 (JP, A) International Publication 89 / 6970 (WO, A1) WO 97/890 (WO, A1) NUTRITION REPORTS INTERNALATION, 1978, Vol. 18, No. 9, pp. 531- 537 Monthly Food Chemical, 1995-2, pp. 45-50 Food Industry, 1993, Vol. 36, pp. 50-56 FOODS AND FOOD IN GREDIENTS JOURNAL OF JAPAN, 1994, No. 159, pp. 65-71 (58) Field surveyed (Int. Cl. 7 , DB name) A61K 38/01 A23K 1/16 A23L 1/30 A23L 1/305 A61K 31/722 A61P 3/06 CA (STN)
Claims (8)
テアーゼ又は酸で加水分解して製造され、平均ペプチド
鎖長が3〜4である脂質代謝改善作用を有するタンパク
質水解物と、キトサンとを有効成分として含有すること
を特徴とする、脂質代謝改善剤。1. An active ingredient comprising a protein hydrolyzate produced by hydrolyzing a protein or a protein-containing substance with a protease or an acid and having an effect of improving lipid metabolism having an average peptide chain length of 3 to 4, and chitosan. An agent for improving lipid metabolism, characterized in that:
配合重量比が4:1〜2:3である請求項1記載の脂質
代謝改善剤。2. The lipid metabolism improving agent according to claim 1, wherein the weight ratio of the protein hydrolyzate to chitosan is from 4: 1 to 2: 3.
配合重量比が3:2である請求項1記載の脂質代謝改善
剤。3. The lipid metabolism improving agent according to claim 1, wherein the weight ratio of the protein hydrolyzate to chitosan is 3: 2.
のいずれか1項に記載の脂質代謝改善剤。4. A dietary lipid absorption inhibitor.
The lipid metabolism improving agent according to any one of the above.
のいずれか1項に記載の脂質代謝改善剤。5. A method for improving postprandial hyperlipidemia.
The lipid metabolism improving agent according to any one of the above.
症の、予防・改善剤である請求項1〜3のいずれか1項
に記載の脂質代謝改善剤。6. The lipid metabolism improving agent according to any one of claims 1 to 3, which is a preventive / ameliorating agent for hyperlipidemia, arteriosclerosis, hypertension, and obesity.
質代謝改善剤を含有する脂質代謝改善用飲食品。7. A food or drink for improving lipid metabolism, comprising the lipid metabolism improving agent according to any one of claims 1 to 3.
質代謝改善剤を含有する脂質代謝改善用動物用飼料。8. An animal feed for improving lipid metabolism, comprising the lipid metabolism improving agent according to any one of claims 1 to 3.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP10066928A JP3108675B2 (en) | 1998-03-17 | 1998-03-17 | Lipid metabolism improver |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP10066928A JP3108675B2 (en) | 1998-03-17 | 1998-03-17 | Lipid metabolism improver |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPH11263733A JPH11263733A (en) | 1999-09-28 |
| JP3108675B2 true JP3108675B2 (en) | 2000-11-13 |
Family
ID=13330147
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP10066928A Expired - Lifetime JP3108675B2 (en) | 1998-03-17 | 1998-03-17 | Lipid metabolism improver |
Country Status (1)
| Country | Link |
|---|---|
| JP (1) | JP3108675B2 (en) |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPH0610163U (en) * | 1992-07-14 | 1994-02-08 | セイコーエプソン株式会社 | Solution container for contact lenses |
| CN101852829B (en) * | 2009-12-30 | 2013-09-11 | 西安开容电子技术有限责任公司 | Insertion loss testing device for lead type filter and design method thereof |
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| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| IT1307278B1 (en) * | 1999-11-18 | 2001-10-30 | Sigma Tau Healthscience Spa | COMPOSITION FOR THE PREVENTION AND / OR TREATMENT OF DISORDERS DUE TO AN ALTERED LIPID METABOLISM, INCLUDING PROPIONIL |
| TWI268138B (en) | 2000-05-11 | 2006-12-11 | Kanebo Seiyaku Ltd | Composition containing peptide and electrolyte excretion enhancing substance, and food containing the same |
| US6991812B2 (en) | 2000-09-05 | 2006-01-31 | Kao Corporation | Agent for preventing, improving or treating hypertension |
| DE10105041A1 (en) * | 2001-02-05 | 2002-08-14 | Tell Pharm Ag Hergiswil | Tripeptides and tripeptide derivatives for the treatment of neurodegenerative diseases |
| GB0211849D0 (en) * | 2002-05-23 | 2002-07-03 | Mok Kenneth H | Improvments to retro-inverso isomers |
| WO2005072750A1 (en) * | 2004-01-30 | 2005-08-11 | Otsuka Pharmaceutical Co., Ltd. | Composition for inhibting dietary lipid absorption |
| JP4982041B2 (en) * | 2004-07-01 | 2012-07-25 | 明治飼糧株式会社 | Method and agent for increasing intramuscular fat (sashi) in livestock |
| KR20070065380A (en) * | 2004-10-08 | 2007-06-22 | 마츠타니 케미컬 인더스트리즈 컴퍼니, 리미티드 | Drug for diminishing increase of neutral fat in blood after meal and food containing the same |
| JP4395658B2 (en) * | 2005-11-17 | 2010-01-13 | エムジーファーマ株式会社 | Composition for inhibiting cholesterol re-elevation and method of use thereof |
| WO2009020189A1 (en) | 2007-08-07 | 2009-02-12 | Mg Pharma Inc. | Anti-hypertensive agent |
| JP6024104B2 (en) * | 2011-12-12 | 2016-11-09 | 学校法人自治医科大学 | Afferent vagus nerve activator, appetite suppressant, fat consumption promoter, fatty liver therapeutic agent, diabetes therapeutic agent, and method for activating afferent vagus nerve in domestic animal species and wild animals excluding humans |
| JP6140763B2 (en) * | 2015-05-18 | 2017-05-31 | 日成興産株式会社 | Specific selective lipid adsorption composition and use thereof |
-
1998
- 1998-03-17 JP JP10066928A patent/JP3108675B2/en not_active Expired - Lifetime
Non-Patent Citations (4)
| Title |
|---|
| FOODS AND FOOD INGREDIENTS JOURNAL OF JAPAN,1994,No.159,pp.65−71 |
| NUTRITION REPORTS INTERNATIONAL,1978,Vol.18,No.9,pp.531−537 |
| 月刊フードケミカル、1995−2、第45−50ページ |
| 食品工業、1993、第36巻、第50−56ページ |
Cited By (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| JPH0610163U (en) * | 1992-07-14 | 1994-02-08 | セイコーエプソン株式会社 | Solution container for contact lenses |
| CN101852829B (en) * | 2009-12-30 | 2013-09-11 | 西安开容电子技术有限责任公司 | Insertion loss testing device for lead type filter and design method thereof |
Also Published As
| Publication number | Publication date |
|---|---|
| JPH11263733A (en) | 1999-09-28 |
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