JP2006151878A - Hypoglycemic agent for diabetes and remedy for hyperlipemia - Google Patents

Hypoglycemic agent for diabetes and remedy for hyperlipemia Download PDF

Info

Publication number
JP2006151878A
JP2006151878A JP2004345134A JP2004345134A JP2006151878A JP 2006151878 A JP2006151878 A JP 2006151878A JP 2004345134 A JP2004345134 A JP 2004345134A JP 2004345134 A JP2004345134 A JP 2004345134A JP 2006151878 A JP2006151878 A JP 2006151878A
Authority
JP
Japan
Prior art keywords
caffeine
curcumin
group
diabetes
extract
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.)
Granted
Application number
JP2004345134A
Other languages
Japanese (ja)
Other versions
JP4604179B2 (en
Inventor
Yukinae Yamazaki
幸苗 山崎
Yasuhiro Kono
泰広 河野
Masami Kamibayashi
正巳 上林
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
National Institute of Advanced Industrial Science and Technology AIST
Original Assignee
National Institute of Advanced Industrial Science and Technology AIST
Priority date (The priority date 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 date listed.)
Filing date
Publication date
Application filed by National Institute of Advanced Industrial Science and Technology AIST filed Critical National Institute of Advanced Industrial Science and Technology AIST
Priority to JP2004345134A priority Critical patent/JP4604179B2/en
Publication of JP2006151878A publication Critical patent/JP2006151878A/en
Application granted granted Critical
Publication of JP4604179B2 publication Critical patent/JP4604179B2/en
Expired - Fee Related legal-status Critical Current
Anticipated expiration legal-status Critical

Links

Images

Abstract

<P>PROBLEM TO BE SOLVED: To provide a hypoglycemic agent for diabetes, having safety and high efficacy, and to provide a remedy for hyperlipemia. <P>SOLUTION: This hypoglycemic agent for the diabetes contains curcumin and further contains one or more kinds of xanthine derivatives selected from caffeine, theophylline, and theobromine. Further, the hypoglycemic agent for the diabetes contains a rhizomatous extract of a plant belonging to the Curcuma genus of the Zingiberaceae family and further contains one or more kinds of the xanthine derivatives selected from the caffeine, the theophylline, and the theobromine. Thus, action only by the curcumin, or only by the extract of the plant belonging to the Curcuma genus of the Zingiberaceae family, is enhanced in the hypoglycemic agent by together using the xanthine derivatives. <P>COPYRIGHT: (C)2006,JPO&NCIPI

Description

本発明は、クルクミンとキサンチン誘導体とを有効成分として含有する、糖尿病血糖降下剤及び高脂血症治療剤に関する。   The present invention relates to a diabetic hypoglycemic agent and an antihyperlipidemic agent containing curcumin and a xanthine derivative as active ingredients.

ショウガ科ウコン属(Curcuma属)植物の根茎はカレー粉の原料として食用とされる他に、健胃、利胆剤等の和漢薬として古くから用いられている。このウコンに含まれる主要な薬理成分の1つはクルクミン(1,7-ビス-(4-ヒドロキシ-3-メトキシフェニル)ヘプタ-1,6-ジエン-3,5-ジオン)であり、抗うつ剤、抗更年期障害剤等(特許文献1参照)や強筋肉剤、抗炎症剤(特許文献2参照)、血流改善組成物(特許文献3参照)、造血器腫瘍の治療薬、免疫抑制剤(特許文献4参照)、老化防止剤(特許文献5)等として利用される他、最近増加の一途をたどっている生活習慣病の予防と治療にも応用されている。 これには、たとえば、2型糖尿病モデルマウスにおける血糖降下作用や(特許文献6参照)、高脂肪食飼育マウスの肝臓におけるトリグリセリド蓄積の抑制作用(特許文献7参照)に基づく薬剤が知られている。   The rhizomes of the ginger family Curcuma genus (Curcuma genus) are used as edible as raw materials for curry powder, and have been used for a long time as a traditional Chinese medicine such as a healthy stomach and galling agent. One of the main pharmacological components contained in this turmeric is curcumin (1,7-bis- (4-hydroxy-3-methoxyphenyl) hepta-1,6-diene-3,5-dione), which is antidepressant Agents, anti-menopausal agents (see Patent Document 1), strong muscle agents, anti-inflammatory agents (see Patent Document 2), blood flow improving compositions (see Patent Document 3), hematopoietic tumor therapeutic agents, immunosuppressants (See Patent Document 4), an anti-aging agent (Patent Document 5), and the like, and also applied to the prevention and treatment of lifestyle-related diseases that have recently been increasing. For example, drugs based on hypoglycemic action in type 2 diabetes model mice (see Patent Document 6) and inhibitory action on triglyceride accumulation in the liver of high-fat diet-fed mice (see Patent Document 7) are known. .

特開2003-113117号公報JP 2003-113117 A 特開2004-182599号公報JP 2004-182599 A 特開2004-123707号公報JP 2004-123707 A 特開2004-75666号公報JP 2004-75666 A 特開2004-2237号公報Japanese Patent Laid-Open No. 2004-2237 特開2003-128539号公報Japanese Patent Laid-Open No. 2003-128539 特開平11-246399号公報Japanese Patent Laid-Open No. 11-246399

しかしながら、クルクミンの当該作用はチアゾリジンジオン等の合成糖尿病薬やフィブレート系の合成抗脂血薬に比べて極めて弱い。しかし、ウコン抽出物やクルクミンは、食材でもあることからわかるように安全性に優れているので、この特徴を活かしながら血糖降下作用等を増強する方法が求められている。   However, the action of curcumin is extremely weak compared to synthetic antidiabetic drugs such as thiazolidinedione and fibrate synthetic antilipidemic drugs. However, turmeric extract and curcumin are excellent in safety, as can be seen from the fact that they are also foodstuffs, and there is a need for a method that enhances the hypoglycemic effect while taking advantage of this feature.

このような状況において、本発明者らは鋭意検討の結果、ウコンやクルクミンの血糖降下作用や中性脂肪減少作用がテオフィリン、カフェイン等、茶やコーヒーに通常含まれるキサンチン誘導体の併用で増強されることを見出し、本発明の完成に至った。すなわち、本発明はクルクミンやクルクミンを含有するウコンエキスを含み、さらにカフェイン、テオフィリン、もしくはテオブロミンの中から選ばれるキサンチン誘導体の1種以上を含有することを特徴とする、糖尿病の血糖降下剤、ないしは高脂血症治療剤に係るものである。   Under these circumstances, as a result of intensive studies, the present inventors have enhanced the blood glucose lowering effect and neutral fat reducing effect of turmeric and curcumin by the combined use of xanthine derivatives usually contained in tea and coffee such as theophylline and caffeine. As a result, the present invention has been completed. That is, the present invention includes curcumin and curcumin-containing turmeric extract, and further contains one or more xanthine derivatives selected from caffeine, theophylline, or theobromine, a hypoglycemic agent for diabetes, Or it relates to a therapeutic agent for hyperlipidemia.

本発明では、クルクミンやウコンエキスによる糖尿病性血糖や血中トリグリセリドあるいは血中総コレステロールの減少がカフェイン等キサンチン誘導体を併用するという簡便な方法で相乗的に強化される。この相乗的な効果はキサンチン誘導体によるホスホジエステラーゼの阻害で生体内セカンドメッセンジャーのcAMPレベルが上昇し、これがクルクミンによるPPAR転写因子群の活性化と共役して脂質・エネルギー代謝の制御因子を増産、活性化するためと考えられる。   In the present invention, diabetic blood glucose, blood triglyceride or blood total cholesterol reduction by curcumin or turmeric extract is synergistically enhanced by a simple method using a xanthine derivative such as caffeine. This synergistic effect is that the inhibition of phosphodiesterase by xanthine derivatives increases the cAMP level of second messenger in the body, which is coupled with the activation of PPAR transcription factors by curcumin to increase production and activation of regulators of lipid and energy metabolism It is thought to do.

このような制御因子としては、その不足が生活習慣病の発症に密接に関わっているサイトカインであるアディポネクチン(非特許文献:下村伊一郎他、実験医学、Vol.20, No.12, 1762- 1767 (2002))が挙げられる。後述の実施例で示されるように、クルクミンとカフェインの同時投与は血糖値の低下と逆相関して血中アディポネクチンの有効濃度を上昇させる。このことは、本発明によるクルクミンとカフェインの両者を含む組成物の糖尿病血糖降下及び高脂血症の改善作用は、アディポネクチンの増強に基づくことを示唆する。 本発明においては、クルクミンとカフェインの両者を含む組成物の糖尿病血糖降下作用及び高脂血症の改善作用が、実際の動物においても発揮され、かつこれらの作用とアディポネクチンの増強作用が関連することを、実際の動物実験レベルで初めて明らかにしたものである。さらに、本発明の有効成分の一つであるカフェイン等も従来から飲食されてきた化合物であるため、これらのコンビネーションによる本発明の薬剤は極めて安全なものといえる。   As such regulatory factors, adiponectin, a cytokine whose deficiency is closely related to the development of lifestyle-related diseases (Non-patent literature: Ichiro Shimomura et al., Experimental Medicine, Vol. 20, No. 12, 1762-1767 ( 2002)). As shown in the Examples described later, simultaneous administration of curcumin and caffeine increases the effective concentration of adiponectin in blood in inverse correlation with the decrease in blood glucose level. This suggests that the diabetic hypoglycemic and hyperlipidemic effects of the composition containing both curcumin and caffeine according to the present invention are based on the enhancement of adiponectin. In the present invention, the diabetic hypoglycemic and hyperlipidemic effects of the composition containing both curcumin and caffeine are also exerted in actual animals, and these actions are related to the adiponectin enhancing action. This is the first time to clarify this at the level of actual animal experiments. Furthermore, since caffeine, which is one of the active ingredients of the present invention, is a compound that has been conventionally eaten and consumed, it can be said that the drug of the present invention based on these combinations is extremely safe.

本発明に用いられるクルクミンはウコン根茎から公知の方法で抽出・精製され、また公知の方法で容易に化学合成もできる。一方、ウコンにはクルクミン以外にも多くの薬理活性化合物が含まれているため、粗抽出物(エキス)としても本発明に好ましく用いられる。このようなエキスの調製には、ウコン(Curcuma longa)や春ウコン(Curcuma aromatica)の根茎を新鮮なままで、もしくは乾燥、細断、粉砕後、エタノール等適当な溶剤で抽出する。抽出物を濃縮し溶媒を除いた残渣はこのままでも用いられるが、活性炭処理やシリカゲルカラムクロマトグラフィー等の公知の手段で不要成分や活性阻害成分を除いてから用いるのも良い。一方、クルクミンやウコンエキスと組み合わせて使用するキサンチン誘導体はテオフィリン、カフェイン、もしくはテオブロミンのいずれか1つまたは2つ以上の混合物である。これらは茶葉やコーヒー豆、カカオ豆等から抽出できるし、公知の方法で容易に合成もできる。   Curcumin used in the present invention is extracted and purified from turmeric rhizomes by a known method, and can be easily chemically synthesized by a known method. On the other hand, since turmeric contains many pharmacologically active compounds in addition to curcumin, it is also preferably used in the present invention as a crude extract (extract). For the preparation of such an extract, the rhizomes of turmeric (Curcuma longa) and spring turmeric (Curcuma aromatica) are kept fresh or dried, chopped and ground, and then extracted with a suitable solvent such as ethanol. The residue obtained by concentrating the extract and removing the solvent can be used as it is, but it may be used after removing unnecessary components and activity-inhibiting components by known means such as activated carbon treatment or silica gel column chromatography. On the other hand, the xanthine derivative used in combination with curcumin or turmeric extract is one or a mixture of two or more of theophylline, caffeine, or theobromine. These can be extracted from tea leaves, coffee beans, cacao beans, etc., and can be easily synthesized by known methods.

また、これらのキサンチン誘導体は当該活性に不都合が無い限り茶葉等原料植物体のままや粗抽出物の状態でも用いることができる。これらのキサンチン誘導体やクルクミン、あるいはそれらの粗抽出物を利用する方法として、エタノールや水に溶解し飲用水に添加する方法、適当なリン脂質等の界面活性剤を含む水に懸濁し飲用水や食物に添加する等の他、適当な補助剤と混合し錠剤の形で利用する方法等が挙げられる。本発明に用いる場合のクルクミン添加量は飲用水の1mlもしくは食物の1gあたり1mgから10mg以下を目安とするが、場合に応じて適宜加減する。ウコンエキスの添加量は精製の方法や程度により生理的に安全な範囲内で所期の効果を得るべく適宜加減する。キサンチン誘導体の添加量については常用されるコーヒーや緑茶に含まれる濃度に準ずるものとする。すなわち、カフェインは飲用水の1mlもしくは食物の1gあたり0.1mgから0.5mg(約3mM)、テオフィリンは飲用水の1mlもしくは食物の1gあたり0.01mgから0.05mg(約0.3 mM)、テオブロミンは飲用水の1mlもしくは食物の1gあたり0.1mgから2mg(約10mM)等を目安にするが、総摂取量や摂取形態に応じて、生理的に安全な範囲内で適宜増減する。次に、本発明を実施例に基づいてさらに詳細に説明する。   In addition, these xanthine derivatives can be used as raw materials such as tea leaves or in the state of a crude extract as long as there is no inconvenience in the activity. As a method of using these xanthine derivatives, curcumin, or a crude extract thereof, a method of dissolving in ethanol or water and adding to drinking water, a method of suspending in water containing a surfactant such as an appropriate phospholipid, In addition to adding to food, there may be mentioned a method of mixing with an appropriate adjuvant and using it in the form of a tablet. The amount of curcumin added for use in the present invention is 1 mg to 10 mg or less per 1 ml of drinking water or 1 g of food, but it may be appropriately adjusted depending on the case. The amount of turmeric extract added is appropriately adjusted in order to obtain the desired effect within a physiologically safe range depending on the method and degree of purification. The amount of xanthine derivative added is in accordance with the concentration contained in commonly used coffee and green tea. Caffeine is 0.1 to 0.5 mg (about 3 mM) per gram of drinking water or 1 g of food, theophylline is 0.01 to 0.05 mg (about 0.3 mM) per liter of drinking water or 1 g of food, and theobromine is drinking water. The standard is 0.1 mg to 2 mg (about 10 mM) per gram of food or 1 g of food, but the dosage should be adjusted appropriately within a physiologically safe range depending on the total intake and intake form. Next, the present invention will be described in more detail based on examples.

〔実施例1〕
遺伝的に2型糖尿病を発症するKK-Ay/Ta Jc1マウス(オス、5週令、17匹、日本クレア社製)をクルクミン及び/又はカフェインを添加し、もしくは添加しないで調製した飼料で4週間にわたり飼育し、体重と摂餌量を定期的に測定し、また1週間に1度採血して血糖値、血中アディポネクチンレベル、血漿トリグリセリド及び総コレステロール濃度を測定した。飼料は日本クレア社製のCE-2粉末飼料の120 gあたりシグマ社製クルクミンのエタノール懸濁液(0.15 g/ml)の4 ml及び/又はカフェイン水溶液(30 mg/ml)の2 mlを加え、さらに2.4 gの馬鈴薯澱粉を水48 mlと混合・加熱して調製したゲルを加え全体を乳鉢と乳棒でよく混和後、直径15 cmのシャーレに固く充填し、その状態で3、4日風乾して調製した固形飼料を自由摂取させた。水は水道水をオートクレーブで滅菌したものを自由摂取させた。 [Example 1]
KK-Ay / Ta Jc1 mice genetically developing type 2 diabetes (male, 5 weeks old, 17 mice, manufactured by Claire Japan) with a feed prepared with or without curcumin and / or caffeine Breeding for 4 weeks, body weight and food consumption were measured regularly, and blood was collected once a week to measure blood glucose level, blood adiponectin level, plasma triglyceride and total cholesterol concentration. The feed is 4 ml of ethanol suspension of Sigma's curcumin (0.15 g / ml) and / or 2 ml of aqueous caffeine (30 mg / ml) per 120 g of CE-2 powder feed made by CLEA Japan. In addition, 2.4 g of potato starch was mixed with 48 ml of water and heated, and the whole was mixed well with a mortar and pestle, and then filled firmly in a petri dish with a diameter of 15 cm. The solid feed prepared by air drying was freely ingested. Water was ingested freely by sterilizing tap water with an autoclave.

血糖やアディポネクチン測定のためのプラズマ(血漿)は、血液をマウス尾部先端から1回あたり9μl採取し、これを直ちに3μlのヘパリン溶液(50 mg/ml)と混合、遠心分離(12000 rpm、12分)で血球を除いて調製した。このプラズマ中のグルコースとトリグリセリド、総コレステロール濃度をそれぞれグルコースCII-テストワコー、トリグリセリドE-テストワコー、コレステロールE-テストワコー(いずれも和光純薬工業株式会社製)で測定した。一方、プラズマの2μlを水8μl及び2x SDS緩衝液の10μlと混合後、95℃で5分加熱処理し、電気泳動の試料とした。ポリアクリルアミドゲルによる電気泳動(各レーン2μlをアプライ)とウェスタンブロッティングによるアディポネクチンの検出は定法によって行った。   Plasma (plasma) for blood glucose and adiponectin measurement is obtained by collecting 9 μl of blood from the tip of the mouse tail, and immediately mixing this with 3 μl of heparin solution (50 mg / ml) and centrifuging (12000 rpm, 12 minutes) ) To remove blood cells. The concentrations of glucose, triglyceride and total cholesterol in the plasma were measured with glucose CII-Test Wako, Triglyceride E-Test Wako and Cholesterol E-Test Wako (all manufactured by Wako Pure Chemical Industries, Ltd.). On the other hand, 2 μl of plasma was mixed with 8 μl of water and 10 μl of 2 × SDS buffer, and then heat-treated at 95 ° C. for 5 minutes to prepare an electrophoresis sample. Detection of adiponectin by electrophoresis using polyacrylamide gel (applying 2 μl of each lane) and Western blotting was performed by a conventional method.

用いた1次抗体はケミコン社製のmouse anti-adiponectin, mouse monoclonal antibody (Catalog No. MAB3608)であり、2次抗体はZymed社製のrabbit anti-mouse Ig G1-HRP conjugate (Catalog No. 61-0120)である。バンドの検出にはPharmacia社製ECL Plus測定キットを用いた。また泳動後のゲルについて、分子量8万前後の部分をCBB試薬で染色し血清アルブミンを検出した。これらのバンドをスキャナーで画像としてパソコンに取り込み、ゲル・プロ・アナライザー(ソフトウェア)でバンドの濃さを数値化した。これらの値から血清アルブミンを基準にした血中アディポネクチンの相対的なレベルを求めた。   The primary antibody used was mouse anti-adiponectin, mouse monoclonal antibody (Catalog No. MAB3608) manufactured by Chemicon, and the secondary antibody was rabbit anti-mouse Ig G1-HRP conjugate (Catalog No. 61- 0120). For detection of the band, an ECL Plus measurement kit manufactured by Pharmacia was used. Moreover, about the gel after electrophoresis, the part with a molecular weight of about 80,000 was dye | stained with the CBB reagent, and serum albumin was detected. These bands were loaded into a personal computer as an image with a scanner, and the density of the band was digitized with Gel Pro Analyzer (software). From these values, the relative level of adiponectin in blood based on serum albumin was determined.

結果を表1、表2、図1〜図3に示す。表1に示すように、各群のマウスの平均体重に有意差はない。表2はクルクミンとカフェインを両方混合した飼料(クルクミン+カフェイン群)では他群より摂食がやや抑制されることを示す。   The results are shown in Table 1, Table 2, and FIGS. As shown in Table 1, there is no significant difference in the average body weight of each group of mice. Table 2 shows that the feed (curcumin + caffeine group) in which both curcumin and caffeine are mixed is somewhat less ingested than the other groups.

Figure 2006151878
注1);クルクミン及び/又はカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの飼育期間中における体重増加を示す。マウスの数はコントロール群で5匹、他の群は各4匹、数値は平均値と標準偏差である。
Figure 2006151878
 Note 1): Shows the increase in body weight during the breeding period of KK-Ay / Ta Jc1 mice raised on a diet supplemented with curcumin and / or caffeine. The number of mice is 5 in the control group, 4 in each of the other groups, and the values are the mean and standard deviation.

Figure 2006151878
注2);クルクミン及び/又はカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの飼育期間中における1日1匹あたりの平均摂餌量を示す。各群の1週間における総摂餌量から計算した。数値は平均値と標準偏差である。
Figure 2006151878
 Note 2): Shows the average amount of food consumed per day during the breeding period of KK-Ay / Ta Jc1 mice raised on a diet supplemented with curcumin and / or caffeine. Calculations were made from the total food intake during one week for each group. Numbers are mean and standard deviation.

図1は血漿中のグルコース濃度は8〜10週令の間クルクミン+カフェイン群で最も低く、糖尿病発症による血糖増加がクルクミンとカフェインの同時投与で最も効果的に抑制されることを示している[各週令ともクルクミン+カフェイン群はコントロール群より有意に低い値を示す(p<0.05)]。図2は9週令と10週令目における血中アディポネクチンの測定結果であるが、コントロール群に比べクルクミンの飼料添加により血中アディポネクチンレベルが上昇し、さらにクルクミンに加えカフェインを添加したクルクミン+カフェイン群では一層上昇することが示された(p<0.05、クルクミン群vs.クルクミン+カフェイン群)。この場合、カフェインのみの添加でもアディポネクチンのレベルはコントロールよりも高値を示したが、図1でカフェイン単独では9,10週令において血糖値がコントロールと同レベルの高値であったことを考えると、血糖降下のために有効なアディポネクチンはクルクミンとの同時投与で増産されると解釈される。さらに、KK-Ay/Taマウスは糖尿病の進行と肥満に伴い血中脂肪も増加するので高脂血症のモデルにもなっている(特開2004-168720)。本実験で血漿トリグリセリドと総コレステロールを測定した結果(図3)では、クルクミン+カフェイン群が最も低い値を示しており、クルクミン単独に比べてクルクミンとカフェインの同時投与が血中脂肪とコレステロール濃度をより減少させた(p<0.05)。   FIG. 1 shows that plasma glucose levels are lowest in the curcumin + caffeine group for 8-10 weeks of age, and that the increase in blood glucose due to the onset of diabetes is most effectively suppressed by simultaneous administration of curcumin and caffeine. [The curcumin + caffeine group shows a significantly lower value than the control group at each age (p <0.05)]. Fig. 2 shows the measurement results of blood adiponectin at 9 and 10 weeks of age. Compared to the control group, the blood adiponectin level increased with the addition of curcumin feed, and curcumin plus caffeine in addition to curcumin + It was shown that the level was further increased in the caffeine group (p <0.05, curcumin group vs. curcumin + caffeine group). In this case, even when only caffeine was added, the level of adiponectin was higher than that of the control, but in FIG. 1, it was considered that the blood glucose level was the same as that of the control at 9, 10 weeks of age with caffeine alone. Adiponectin, which is effective for lowering blood sugar, is interpreted to be increased by co-administration with curcumin. Furthermore, KK-Ay / Ta mice are also models of hyperlipidemia because blood fat increases with the progression of diabetes and obesity (Japanese Patent Laid-Open No. 2004-168720). In the results of the measurement of plasma triglycerides and total cholesterol in this experiment (Fig. 3), the curcumin + caffeine group showed the lowest value. Compared with curcumin alone, simultaneous administration of curcumin and caffeine resulted in blood fat and cholesterol. The concentration was further reduced (p <0.05).

〔実施例2〕
ウコン根茎の乾燥粉末(小西製薬製)200 gを1リットルのへキサンと混合し、室温においてマグネチックスターラーで2日間攪拌後、ウコン粉末を濾集し、アセトンとヘキサンの1:1の混合液1リットルでさらに1日間攪拌、抽出した。粉末を濾別した抽出液をロータリーエバポレーターで濃縮後、オイルポンプで減圧乾燥し、油状物11.1gを得た。 [Example 2]
200 g of dried turmeric rhizome powder (manufactured by Konishi Pharmaceutical) is mixed with 1 liter of hexane, stirred for 2 days at room temperature with a magnetic stirrer, turmeric powder is collected by filtration, and a 1: 1 mixture of acetone and hexane The mixture was further stirred and extracted for 1 day with 1 liter. The extract obtained by filtering the powder was concentrated with a rotary evaporator and dried under reduced pressure with an oil pump to obtain 11.1 g of an oily substance.

〔実施例3〕
KK-Ay/Ta Jc1マウス(オス、5週令、10匹)を、実施例2で調製したウコンエキス又はウコンエキスとカフェインを添加した飼料、もしくはこれらを添加しない飼料で4週間にわたり飼育し、体重、摂餌量、血糖値を定期的に測定した。飼料はCE-2粉末飼料120 gあたり上記ウコンエキスのエタノール溶液(0.2 g/ml)の1.2 ml、又は同エタノール溶液の1.2 mlとカフェイン水溶液(30 mg/ml)の2 ml、もしくはエタノールのみの1.2 mlを加え、乳鉢でよく混和調製した粉末飼料を自由摂取させた。水は水道水をオートクレーブで滅菌したものを自由摂取させた。血糖値はマウス尾部から微量採血しグルコースセンサー(三和化学研究所製グルテストNeoセンサー)を用いて測定した。結果を表3、表4、図4に示す。

Figure 2006151878
注3);ウコンエキスとカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの飼育期間中における体重増加を示す。マウスの数はコントロール群とウコンエキス+カフェイン群で各3匹、ウコンエキス群で4匹、数値は平均値と標準偏差である。
Figure 2006151878
 注4);ウコンエキスとカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの飼育期間中における1日1匹あたりの平均摂餌量を示す。各群の1週間における総摂餌量から計算した。数値は平均値と標準偏差である。

表3に示すように、ウコンエキスのみの群では体重増加がコントロール群より大きかったが、ウコンエキス+カフェイン群はコントロール群との間に大きな差はなかった。一方、摂餌量(表4)については、ウコンエキス+カフェイン群がコントロール群に比べてわずかながら減少傾向を示した。図4は血糖測定の結果であるが、8、9週令目の血糖値がコントロール群やウコンエキス群に比べウコンエキス+カフェイン群で顕著に減少していることを示す。 Example 3
KK-Ay / Ta Jc1 mice (male, 5 weeks old, 10 mice) were bred for 4 weeks with the turmeric extract prepared in Example 2, the feed with added turmeric extract and caffeine, or the feed without these added. Body weight, food intake and blood glucose level were measured regularly. The feed is 1.2 ml of the above turmeric extract ethanol solution (0.2 g / ml) per 120 g of CE-2 powder feed, or 1.2 ml of the same ethanol solution and 2 ml of caffeine aqueous solution (30 mg / ml), or ethanol only 1.2 ml of was added, and the powdered feed mixed well in the mortar was ingested freely. Water was ingested freely by sterilizing tap water with an autoclave. The blood glucose level was measured by using a glucose sensor (Glutest Neo sensor manufactured by Sanwa Chemical Laboratory) after collecting a small amount of blood from the tail of the mouse. The results are shown in Table 3, Table 4, and FIG.
Figure 2006151878
 Note 3): Shows the increase in body weight during the breeding period of KK-Ay / Ta Jc1 mice raised on feed supplemented with turmeric extract and caffeine. The number of mice is 3 for each of the control group and the turmeric extract + caffeine group, 4 for the turmeric extract group, and the numerical values are the mean and standard deviation.
Figure 2006151878
 Note 4): Shows the average amount of food consumed per day during the breeding period of KK-Ay / Ta Jc1 mice fed with feed supplemented with turmeric extract and caffeine. Calculations were made from the total food intake during one week for each group. Numbers are mean and standard deviation.

As shown in Table 3, the weight gain was greater in the turmeric extract alone group than in the control group, but the turmeric extract + caffeine group was not significantly different from the control group. On the other hand, as for food intake (Table 4), the turmeric extract + caffeine group showed a slightly decreasing tendency compared to the control group. FIG. 4 shows the results of blood glucose measurement, and shows that blood glucose levels at 8 and 9 weeks of age are significantly decreased in the turmeric extract + caffeine group compared to the control group and the turmeric extract group.

〔実施例4〕
KK-Ay/Ta Jc1マウス(オス、5週令、13匹)を、実施例2で調製したウコンエキス又はそれとカフェインとを添加し実施例1と同様に固形とした飼料[ウコンエキス添加量はCE-2粉末の0.3%(w/w)]もしくはこれらを添加しない固形飼料で4週間にわたり飼育し、体重、摂餌量、血漿トリグリセリド濃度を定期的に測定した(コントロール群とウコンエキス群は各4匹、ウコンエキス+カフェイン群は5匹)。体重と摂餌量の変化は実施例3の結果と類似していた。血漿トリグリセリド濃度の測定結果を図5に示すが、血中脂肪の増加がウコンエキス群に比べ、ウコンエキス+カフェイン群ではより強く抑制される傾向が認められた(p<0.05、8週令目コントロール群vs.ウコンエキス群;p<0.10、同ウコンエキス群vs.ウコンエキス+カフェイン群)。 Example 4
KK-Ay / Ta Jc1 mice (male, 5 weeks old, 13 mice) were added with the turmeric extract prepared in Example 2 or it and caffeine, and the feed was solidified in the same manner as in Example 1 [Additional amount of turmeric extract Is 0.3% (w / w) of CE-2 powder] or solid feed without these supplements for 4 weeks, and body weight, food intake and plasma triglyceride concentration were measured regularly (control group and turmeric extract group) 4 each, 5 in turmeric extract + caffeine group). The changes in body weight and food intake were similar to the results of Example 3. The results of measurement of plasma triglyceride concentration are shown in FIG. 5. The increase in blood fat tended to be more strongly suppressed in the turmeric extract + caffeine group than in the turmeric extract group (p <0.05, 8 weeks old). Eye control group vs. turmeric extract group; p <0.10, turmeric extract group vs. turmeric extract + caffeine group).

〔実施例5〕
別の2型糖尿病モデルマウス(BKS.Cg-+Leprdb/+Leprdb /Jc1、日本クレア製、6週令、12匹)を実施例1と同様にクルクミン及び/又はカフェインを添加し、もしくは添加しないで調製した固形飼料で4週間にわたり飼育し、体重、摂餌量、血糖値を定期的に測定した(合計4群で各群3匹)。体重と摂餌量は各群で顕著な違いはなかった。血漿グルコース濃度の測定結果を図6に示すが、クルクミンとカフェインの同時投与群は各週令を通じてコントロール群よりも低い値を示し、また10週令目にはクルクミン単独投与群よりも低い値(p<0.05)を示した。 Example 5
Another type 2 diabetes model mouse (BKS.C g- + Lepr db / + Lepr db / Jc1, manufactured by CLEA Japan, 6 weeks old, 12 mice) was added with curcumin and / or caffeine in the same manner as in Example 1. The animals were reared for 4 weeks on a solid feed prepared without or added, and body weight, food intake, and blood glucose level were measured regularly (3 animals in 4 groups in total). There was no significant difference in body weight and food intake between groups. The measurement results of plasma glucose concentration are shown in FIG. 6. The group administered simultaneously with curcumin and caffeine showed a lower value than the control group throughout each week, and was lower than the group administered with curcumin alone at 10 weeks of age ( p <0.05).

クルクミン及び/又はカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの8〜10週令における血糖値を測定した結果を示すグラフである。図中、棒グラフは平均値、エラーバーは標準偏差、n = 9〜12である。It is a graph which shows the result of having measured the blood glucose level in 8-10 weeks old of the KK-Ay / Ta Jc1 mouse reared with the feed which added curcumin and / or caffeine. In the figure, the bar graph is the average value, the error bar is the standard deviation, and n = 9-12. クルクミン及び/又はカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの9及び10週令における血中アディポネクチンレベルを測定した結果を示すグラフである。図中、棒グラフは平均値、エラーバーは標準偏差、n = 13〜29である。It is a graph which shows the result of having measured the blood adiponectin level in 9 and 10-week-old of the KK-Ay / Ta Jc1 mouse reared with the feed which added curcumin and / or caffeine. In the figure, the bar graph is the average value, the error bar is the standard deviation, and n = 13 to 29. クルクミン及び/又はカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの9及び10週令における血漿トリグリセリド濃度(A)及び総コレステロール濃度(B)を測定した結果を示すグラフである。図中、棒グラフは平均値、エラーバーは標準偏差、n = 9〜12である。It is a graph which shows the result of having measured the plasma triglyceride density | concentration (A) and the total cholesterol density | concentration (B) in 9 and 10-week-old of the KK-Ay / Ta Jc1 mouse | mouth raised with the feed which added curcumin and / or caffeine. In the figure, the bar graph is the average value, the error bar is the standard deviation, and n = 9-12. ウコンエキスとカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの6〜9週令における血糖値を測定した結果を示すグラフである。図中、棒グラフは平均値、エラーバーは標準偏差、n = 4,3である。It is a graph which shows the result of having measured the blood glucose level in 6-9 weeks old of the KK-Ay / Ta Jc1 mouse | mouth raised with the feed which added the turmeric extract and caffeine. In the figure, the bar graph is the average value, the error bar is the standard deviation, and n = 4,3. ウコンエキスとカフェインを添加した飼料で飼育したKK-Ay/Ta Jc1マウスの7〜9週令における血漿トリグリセリド濃度を示すグラフである。図中、棒グラフは平均値、エラーバーは標準偏差、n = 8〜15である。It is a graph which shows the plasma triglyceride density | concentration in 7-9 week-old of the KK-Ay / Ta Jc1 mouse | mouth raised with the feed which added the turmeric extract and caffeine. In the figure, the bar graph is the average value, the error bar is the standard deviation, and n = 8-15. ウコンエキスを添加した飼料で飼育したBKS.Cg-+Leprdb/+Leprdb /Jc1マウスの7〜10週令における血糖値を示すグラフである。図中、棒グラフは平均値、エラーバーは標準偏差、n = 6〜9である。It is a graph showing the blood glucose levels in BKS.C g- + Lepr db / + Lepr 7~10 weeks old db / Jc1 mice fed with diets supplemented with turmeric extract. In the figure, the bar graph is the average value, the error bar is the standard deviation, and n = 6-9.

Claims (4)

クルクミンを含み、さらにカフェイン、テオフィリン、もしくはテオブロミンの中から選ばれるキサンチン誘導体の1種以上を含有することを特徴とする糖尿病血糖降下剤。   A diabetic hypoglycemic agent comprising curcumin and further containing one or more xanthine derivatives selected from caffeine, theophylline, or theobromine. ショウガ科ウコン属(Curcuma属)植物の根茎抽出物を含み、さらにカフェイン、テオフィリン、もしくはテオブロミンの中から選ばれるキサンチン誘導体の1種以上を含有することを特徴とする糖尿病血糖降下剤。   A diabetic hypoglycemic agent comprising a rhizome extract of a ginger family Curcuma genus, and further containing one or more xanthine derivatives selected from caffeine, theophylline, or theobromine. クルクミンを含み、さらにカフェイン、テオフィリン、もしくはテオブロミンの中から選ばれるキサンチン誘導体の1種以上を含有することを特徴とする高脂血症治療剤。   A therapeutic agent for hyperlipidemia, comprising curcumin, and further containing at least one xanthine derivative selected from caffeine, theophylline, or theobromine. ショウガ科ウコン属(Curcuma属)植物の根茎抽出物を含み、さらにカフェイン、テオフィリン、もしくはテオブロミンの中から選ばれるキサンチン誘導体の1種以上を含有することを特徴とする、高脂血症治療剤

A therapeutic agent for hyperlipidemia, comprising a rhizome extract of a turmeric genus Curcuma, further containing at least one xanthine derivative selected from caffeine, theophylline, or theobromine

JP2004345134A 2004-11-30 2004-11-30 Diabetic hypoglycemic agent and antihyperlipidemic agent Expired - Fee Related JP4604179B2 (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
JP2004345134A JP4604179B2 (en) 2004-11-30 2004-11-30 Diabetic hypoglycemic agent and antihyperlipidemic agent

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
JP2004345134A JP4604179B2 (en) 2004-11-30 2004-11-30 Diabetic hypoglycemic agent and antihyperlipidemic agent

Publications (2)

Publication Number Publication Date
JP2006151878A true JP2006151878A (en) 2006-06-15
JP4604179B2 JP4604179B2 (en) 2010-12-22

Family

ID=36630593

Family Applications (1)

Application Number Title Priority Date Filing Date
JP2004345134A Expired - Fee Related JP4604179B2 (en) 2004-11-30 2004-11-30 Diabetic hypoglycemic agent and antihyperlipidemic agent

Country Status (1)

Country Link
JP (1) JP4604179B2 (en)

Cited By (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JP2008120726A (en) * 2006-11-10 2008-05-29 Univ Nagoya Anti-ageing transcription factor-activating agent and utilization thereof
WO2011144545A1 (en) 2010-05-19 2011-11-24 Unilever Nv Theobromine for increasing hdl-cholesterol

Families Citing this family (2)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
KR101381850B1 (en) 2012-11-01 2014-04-10 (주)휴럼 Composition comprising curcuma longa extract having anti-cholesterol activities and the method curcuma longa extract
KR102000703B1 (en) * 2018-01-17 2019-07-16 이창호 Composition for controlling Blood Sugar comprising Fermented Fluid of Iceplant and Manufacturing method thereof

Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JPH11246399A (en) * 1998-03-03 1999-09-14 Lion Corp Lipid metabolism improving composition
WO2002049699A2 (en) * 2000-12-21 2002-06-27 Kimberly-Clark Worldwide, Inc. Respiratory suction catheter apparatus with antimicrobial chamber
US20030007996A1 (en) * 2001-05-30 2003-01-09 Graham Terry E. Therapies for the prevention and treatment of diabetes and obesity
JP2003128539A (en) * 2001-10-23 2003-05-08 Kanegafuchi Chem Ind Co Ltd Peroxisome proliferative agent-responding receptor ligand agent

Patent Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JPH11246399A (en) * 1998-03-03 1999-09-14 Lion Corp Lipid metabolism improving composition
WO2002049699A2 (en) * 2000-12-21 2002-06-27 Kimberly-Clark Worldwide, Inc. Respiratory suction catheter apparatus with antimicrobial chamber
US20030007996A1 (en) * 2001-05-30 2003-01-09 Graham Terry E. Therapies for the prevention and treatment of diabetes and obesity
JP2003128539A (en) * 2001-10-23 2003-05-08 Kanegafuchi Chem Ind Co Ltd Peroxisome proliferative agent-responding receptor ligand agent

Cited By (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
JP2008120726A (en) * 2006-11-10 2008-05-29 Univ Nagoya Anti-ageing transcription factor-activating agent and utilization thereof
WO2011144545A1 (en) 2010-05-19 2011-11-24 Unilever Nv Theobromine for increasing hdl-cholesterol
US11806352B2 (en) 2010-05-19 2023-11-07 Upfield Europe B.V. Theobromine for increasing HDL-cholesterol

Also Published As

Publication number Publication date
JP4604179B2 (en) 2010-12-22

Similar Documents

Publication Publication Date Title
US9573919B2 (en) Peroxisome proliferator-activated receptor (PPAR) activator, and drugs, supplements, functional foods and food additives using the same
CN104220084B (en) Include prevention or treatment pharmaceutical composition of the Rhizoma Smilacis Glabrae extract as the obesity of active ingredient, hyperlipidemia or fatty liver
JP2008273938A (en) Adiponectin production-promoting agent
KR100883356B1 (en) Compositions for Improving Obesity
JP4834824B2 (en) Adiponectin production enhancer
JPWO2005115366A1 (en) Lifestyle-related disease prevention / amelioration agent containing turmeric essential oil component
JPWO2010134373A1 (en) Preventive and / or therapeutic agent for metabolic syndrome
KR101558476B1 (en) Novel Use of Filvertone
JP2006131578A (en) Extract obtained from plant body of lotus, method for producing the extract and obesity inhibitor
JP2011207776A (en) Adiponectin production-promoting agent
JP4604179B2 (en) Diabetic hypoglycemic agent and antihyperlipidemic agent
JP6913402B2 (en) A combination drug suitable for the treatment and prevention of non-alcoholic steatohepatitis (NASH)
JP2023157951A (en) Composition for improving liver function
JP4974553B2 (en) Acetaldehyde metabolism promoter
Shelke et al. Review on dhatryadi churna: An ayurvedic antipyretic polyherbal formulation
JP2011168540A (en) Anti-obesity action promoter, and adiponectin secretion promoter or inhibitor of reduction in the secretion of adiponectin
JP2007297370A (en) Suppressor of increase in blood glucose level
JP6144564B2 (en) Inflammation prevention agent
EP2067478A1 (en) Agent for prevention or treatment of blood glucose level elevation
KR101101808B1 (en) Novel uses of adipic acid
JP5122924B2 (en) Anti-obesity agent
JP4863327B2 (en) Adiponectin production enhancer
WO2007116980A1 (en) Suppressor of increase in blood glucose level
JP2015078140A (en) Prevention/treatment agent for alcoholic fatty liver
KR100992995B1 (en) Novel uses of piperonal

Legal Events

Date Code Title Description
A621 Written request for application examination

Free format text: JAPANESE INTERMEDIATE CODE: A621

Effective date: 20061101

A131 Notification of reasons for refusal

Free format text: JAPANESE INTERMEDIATE CODE: A131

Effective date: 20100615

A521 Request for written amendment filed

Free format text: JAPANESE INTERMEDIATE CODE: A523

Effective date: 20100804

A521 Request for written amendment filed

Free format text: JAPANESE INTERMEDIATE CODE: A821

Effective date: 20100809

TRDD Decision of grant or rejection written
A01 Written decision to grant a patent or to grant a registration (utility model)

Free format text: JAPANESE INTERMEDIATE CODE: A01

Effective date: 20100907

A01 Written decision to grant a patent or to grant a registration (utility model)

Free format text: JAPANESE INTERMEDIATE CODE: A01

A61 First payment of annual fees (during grant procedure)

Free format text: JAPANESE INTERMEDIATE CODE: A61

Effective date: 20100908

R150 Certificate of patent or registration of utility model

Free format text: JAPANESE INTERMEDIATE CODE: R150

FPAY Renewal fee payment (event date is renewal date of database)

Free format text: PAYMENT UNTIL: 20131015

Year of fee payment: 3

FPAY Renewal fee payment (event date is renewal date of database)

Free format text: PAYMENT UNTIL: 20131015

Year of fee payment: 3

R250 Receipt of annual fees

Free format text: JAPANESE INTERMEDIATE CODE: R250

LAPS Cancellation because of no payment of annual fees