KR100573590B1 - New Herbal Composition for Treatment and Prevention of Obesity - Google Patents
New Herbal Composition for Treatment and Prevention of Obesity Download PDFInfo
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- KR100573590B1 KR100573590B1 KR1020040006785A KR20040006785A KR100573590B1 KR 100573590 B1 KR100573590 B1 KR 100573590B1 KR 1020040006785 A KR1020040006785 A KR 1020040006785A KR 20040006785 A KR20040006785 A KR 20040006785A KR 100573590 B1 KR100573590 B1 KR 100573590B1
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Abstract
본 발명은 길경(Platycodi radix) 추출물 1.0 중량부, 귤피(Citrus unshiu Markovich) 추출물 0.8~1.2 중량부, 백모근(Imperatae rhizoma) 추출물 1.4~3.5 중량부 및 맥문동(Liriopsis tuber) 추출물 1.1~1.7 중량부의 혼합물을 함유하는 생약 조성물 및 이를 유효성분으로 함유하는 비만억제 및 비만치료용 약제 및 건강기능식품에 관한 것이다.The present invention is a mixture of 1.0 parts by weight of Platycodi radix extract, 0.8 to 1.2 parts by weight of Citrus unshiu Markovich extract, 1.4 to 3.5 parts by weight of Imperatae rhizoma extract and 1.1 to 1.7 parts by weight of Liriopsis tuber extract. It relates to a herbal composition containing and an anti-obesity and obesity treatment pharmaceuticals and health functional foods containing the same as an active ingredient.
본 발명에 의하여, 사용자의 거부감이 없고 다른 부작용이 없는 우수한 천연 물 유래의 비만억제 및 비만치료용 약제 또는 건강기능식품을 제공하는 것이 가능하게 된다.According to the present invention, it is possible to provide an excellent natural water-derived obesity suppression and obesity treatment agent or health functional food without user's rejection and other side effects.
비만억제, 비만치료, 생약, 조성물, 추출, 고지혈증, 길경, 귤피, 백모근, 맥문동Obesity Inhibition, Obesity Treatment, Herbal Medicine, Composition, Extract, Hyperlipidemia, Gil-Gyeong, Gyulpi, White Hair Root, Macmundong
Description
도 1 은 본 발명에 의한 생약 조성물이 세포의 β3AR 활성에 미치는 효과를 보여주는 전기영동 사진 및 도표.1 is an electrophoretic photograph and a diagram showing the effect of the herbal composition according to the present invention on the β3AR activity of the cells.
본 발명은 길경(Platycodi radix), 귤피(Citrus unshiu Markovich), 맥문동(Liriopsis tuber) 및 백모근(Imperatae rhizoma)의 혼합물로부터 추출하여 수득되는 비만치료ㆍ억제용 생약 조성물에 관한 것이다.The present invention relates to a herbal composition for treating and suppressing obesity obtained by extracting from a mixture of Platycodi radix , Citrus unshiu Markovich , Liriopsis tuber , and Imperatae rhizoma .
최근 경제의 현대화에 따른 생활 수준의 향상으로 지방과 당분의 섭취는 늘고 섬유질의 섭취는 줄어드는 새로운 식사 문화, 특히 외식 문화의 정착으로 고단백 위주의 식단 선호 현상이 두드러지고 있으며, 이에 반하여 육체적인 활동이 거의 없는 현대인의 생활 습관으로 비만 인구가 급속히 늘고 있는 것이 현실이다. 고열량 식품의 섭취가 증가하고 섬유질 섭취가 줄어들면서 비만, 특히 복부비만이 사회적으로 심각한 문제로 떠오르고 있는 것이다. 비만은 지방조직이 과잉 증가한 상태를 말하며 비만에 의한 체중의 증가는 대부분 지방의 증가에 기인하는 것이다.Recently, with the improvement of living standards due to the modernization of the economy, a new dietary culture, in which fat and sugar intake is increased and fiber intake is reduced, especially eating out, has become a preference for high protein-oriented diets. The reality is that the obese population is rapidly increasing due to the few lifestyles of modern people. As the consumption of high-calorie foods increases and fiber intake decreases, obesity, especially abdominal obesity, is becoming a serious social problem. Obesity refers to a state in which fat tissue is excessively increased, and weight gain due to obesity is mostly due to an increase in fat.
비만의 유해성은 비만 그 자체로 지방조직에 의한 복부의 압박으로 인하여 변비와 소화불량, 위장장해 등을 일으키는 경우가 많을 뿐만 아니라, 이로 인해 많은 성인병들의 위험요소가 된다는데 문제가 있다. 비만은 암을 비롯한 동맥경화, 심장병, 고혈압, 당뇨병 등과 같은 성인병과 합병증을 일으키는 등 만병의 근원이라고 알려져 있으며 1996년 세계보건기구(WHO)도 비만은 치료가 필요한 병이라고 경고한 바 있다. 75만명을 대상으로 한 연구에 의하면 평균 체중보다 40% 이상인 남성과 여성에서 정상 체중인 사람들 보다 사망률이 1.9배 증가된 것으로 조사되었다. Obesity is a problem that obesity itself causes a lot of constipation, indigestion, gastrointestinal disorders due to the pressure of the abdomen by the fat tissue, as well as the risk factors of many adult diseases. Obesity is known to cause all kinds of complications such as cancer, arteriosclerosis, heart disease, high blood pressure, diabetes and other complications, and in 1996, the World Health Organization (WHO) warned that obesity is a disease that needs treatment. A study of 750,000 people reported a 1.9-fold increase in mortality in men and women who were 40% or more above average body weight than those of normal weight.
비만은 신체에 지방이 과잉되게 축적된 상태이며, 지방이 체내에 축적되는 원인은 당질(탄수화물)의 과잉섭취 또는 지방을 과잉섭취 하는 데 있다. 비만에 달하는 메카니즘은 당질을 과잉 섭취함으로써 음식물 중에 함유되어있는 당질이 소화되어 단당이 되고 소장을 통해 체내로 흡수되며, 혈당이 상승하여 그 자극으로 분비되는 인슐린이 지방세포에 작용해서 혈액 중의 단당을 지방세포가 받아들이게 되어 지방으로 바꾸는 것이다. 또한 식품성분 중 가장 고칼로리인 지방(트리글리세리드)은 췌(膵) 리파아제에 의해 분해되어 소장을 통해 흡수되며, 섭취 칼로리의 과잉으로 저장 칼로리가 증가되는 결과가 된다. 즉, 과잉 지방섭취에 의해 비만이 되는 것이다.Obesity is a state in which excess fat is accumulated in the body, and the cause of fat accumulation in the body is excessive intake of sugar (carbohydrate) or excess intake of fat. The mechanism of reaching obesity is that by over-ingesting the sugars, the sugars in the food are digested and become monosaccharides and absorbed into the body through the small intestine.Increase the blood sugar and insulin secreted by the stimulus acts on fat cells to release the monosaccharides in the blood. Fat cells are taken in and converted into fat. In addition, fat (triglyceride), which is the highest calorie among food ingredients, is broken down by pancreatic lipase and absorbed through the small intestine, resulting in an increase in stored calories due to excess calories. That is, obesity is caused by excess fat intake.
따라서 비만을 유발하는 이들의 어떤 경로의 일부분을 저해함으로써 항비만 작용을 발생시키려는 생각을 바탕으로 현재 각종 항비만제에 관한 연구가 진행되고 있다. Therefore, studies on various anti-obesity agents are currently being conducted based on the idea of generating anti-obesity effects by inhibiting a part of certain pathways that cause obesity.
당질 과잉섭취로 비만이 되는 경로를 저해하는 당질분해 소화효소저해작용, 혈당상승 억제작용, 또는 단당흡수 억제작용에 의해 또는 지방 과잉 섭취에 의해 비만에 달하는 경로를 저해하는 콜산 흡착 배설작용, 콜레스테롤 저하작용, 혈중 트리글리세리드 저하작용, 또는 리파아제 저해작용에 의해 비만을 예방 및 개선할 수 있다고 생각되어, 이들 작용을 가지는 의약성분에 대한 연구가 계속하여 진행되고 있다.Cholesterol adsorption excretion, cholesterol lowering, inhibiting glycolysis digestive enzyme inhibition, hyperglycemia inhibition, or monosaccharide absorption inhibition or excess fat ingestion It is thought that obesity can be prevented and improved by the action, the blood triglyceride lowering action, or the lipase inhibitory action, and the research on the pharmaceutical component which has these actions is continuing.
탄수화물(당질)의 과잉섭취로 인한 급격한 식후 혈당상승과 과다한 인슐린 분비는, 비만 외에도 당뇨병 혹은 고지혈증을 야기하며(약리와 치료 Vol. 19, No. 10 Oct. 274, 1991), 당질분해 소화효소를 저해함으로써 당뇨병 혹은 고지혈증도 예방 및 개선할 수 있다고 알려져 있다. 따라서 당질분해 소화효소 저해제, 단당흡수 억제제, 또는 혈당상승 억제제는 항당뇨병제, 항고지혈증제, 또는 항동맥경화증제로 유용하다고 생각된다. 현재 의약품으로 사용되고 있는 당질분해 소화효소 저해제로는 α-글루코시다아제 저해제인 아카보스(Acarbose, 바이엘약품 주식회사)나 식후 과혈당 개선제인 보그리보오즈(AO-128, 다께다약품 주식회사)가 있다. 이들은 동물시험이나 임상시험에서 식후 혈당치의 상승 억제효과가 확인되었고, 항비만, 항당뇨병에 대한 유효성도 보고되었다(Res. Exp. Med.vol. 175, 87(1979), 일본 농예화학회지 vol. 63, 217(1989), New Current vol. 6, 2(1995)].Rapid postprandial blood sugar rise and excessive insulin secretion due to excessive intake of carbohydrates (sugars) can lead to diabetes or hyperlipidemia in addition to obesity (Pharmacology and Treatment Vol. 19, No. 10 Oct. 274, 1991), Inhibition is known to prevent and improve diabetes or hyperlipidemia. Therefore, glycosylated digestive enzyme inhibitors, monosaccharide absorption inhibitors, or blood glucose elevation inhibitors are considered to be useful as antidiabetic agents, antihyperlipidemic agents, or antiarteriosclerosis agents. Glycolytic digestive enzyme inhibitors currently used in medicine include acarbose (Acarbose, Bayer Pharmaceutical Co., Ltd.) and Bogriboose (AO-128, Daeda Pharmaceutical Co., Ltd.), a post-prandial hyperglycemic improver. In animal studies or clinical trials, the effect of suppressing postprandial blood sugar levels was confirmed, and the effectiveness of anti-obesity and anti-diabetic disease was also reported (Res. Exp. Med. Vol. 175, 87 (1979), Japanese Journal of Agricultural Chemistry vol. 63, 217 (1989), New Current vol. 6, 2 (1995).
또한 지방(트리글리세리드) 섭취로 비만에 달하는 경로를 저해하는 방법으로는 콜산 흡착 배설, 콜레스테롤 저하, 혈중 트리글리세리드 저하, 리파아제 저해 등이 있다. 콜산 배설작용을 가지는 의약으로는 고콜레스테롤 혈증치료제인 콜레스티라민(colestyramine)이 있고, 이것은 음이온교환수지이다. 음이온 교환수지를 경구투여하는 것에 의해 음이온 교환수지는 장간순환(腸肝循環)(마끼노 이사오라, 다이샤, vol. 24, No. 8, 685-692, 1987)하고 있는 장내의 콜산을 흡착고정하여 콜산의 재흡수를 방해하고, 간장에서 콜레스테롤의 콜산으로의 변환을 촉진시켜, 그 결과 혈중 콜레스테롤 농도를 저하시키는 작용을 가진다. 그러나, 콜레스티라민의 용법이 9 g을 100 mL의 물에 현탁해서 복용하게 되어 있어서, 1 회 투여량이 매우 많고, 복용 시에는 수지의 거칠거칠한 불괘한 감촉이 입안에 남아서 환자가 무척 복용하기 어렵다는 문제점이 있었다.In addition, fat (triglyceride) intake to inhibit the path to obesity, such as exclusion of cholic acid adsorption, cholesterol lowering, blood triglyceride lowering, lipase inhibition and the like. Drugs with cholic acid excretion include cholstyramine, a hypercholesterolemic drug, which is an anion exchange resin. By oral administration of the anion exchange resin, the anion exchange resin adsorbs cholic acid in the intestinal circulatory organs (Makino Isaora, Taisha, vol. 24, No. 8, 685-692, 1987). Fixing interferes with the resorption of cholic acid and promotes the conversion of cholesterol into cholic acid in the liver, resulting in a lowering of cholesterol levels in the blood. However, the usage of cholestyramine is to take 9 g in 100 mL of water, so the dose is very high, and when taken, the rough uncomfortable texture of the resin remains in the mouth, which is very often taken by the patient. There was a difficult problem.
상기와 같이 각각의 작용을 가지는 수많은 화학 합성 화합물이 보고 되고, 의약품으로 사용되고 있지만, 이들은 복용량이 많다거나 복용 시에 불쾌감이 있다는 문제점이 있으며, 또한 화학 합성 화합물이기 때문에 투여시에 피험자가 인체에 대한 안전성에 불안을 느끼는 경우가 있었다. As described above, a number of chemical synthetic compounds having respective actions have been reported and used as medicines, but these have a problem in that they have a high dose or are unpleasant at the time of taking them, and because they are chemically synthesized compounds, the test subjects have no effect on the human body at the time of administration. In some cases, safety was anxiety.
비만억제와 변비개선을 위해서는 음식물, 특히 고열량 식품의 섭취를 줄이고, 에너지 소비를 늘림으로써 지방의 체내축적을 억제시키는 것이 중요하다. 특히 음식물 섭취의 감소보다는 에너지 소비를 증가시키는 것이 비만억제에 효과적이라고 알려져 있다. 규칙적인 운동은 에너지 소비를 증가시켜 심혈관계 질환으로 인한 사망률을 크게 낮출 수 있다는 보고도 있다. 그러나 지속적으로 운동하기 어려운 현대사회의 특성으로 인해 비만억제를 위한 주된 노력은 비만억제 및 변비개선 효과가 있는 천연소재 유래의 약제, 다이어트 식품이나 건강 기능식품의 섭취에 초점이 맞춰져 있어 이와 관련된 많은 제품들이 개발·시판되고 있다.In order to suppress obesity and improve constipation, it is important to reduce the body's accumulation of fat by reducing the consumption of food, especially high-calorie foods, and increasing energy consumption. In particular, increasing energy consumption rather than reducing food intake is known to be effective in suppressing obesity. Regular exercise has also been shown to increase energy consumption and significantly reduce mortality from cardiovascular disease. However, due to the nature of the modern society, which is difficult to continuously exercise, the main efforts to control obesity are focused on the consumption of drugs derived from natural materials, diet foods, or dietary supplements that are effective in suppressing obesity and improving constipation. Are developed and marketed.
특히 의이인(Cocis semen), 산약(Dioscoreae rhizoma), 길경(Platycodi radix)(도라지), 오미자(Schizandrae fructus), 귤피(Citrus unshiu Markovich), 알로에(Aloe vera), 산더덕(Adenophorae radix; 사삼) 등 몇 가지 생약 단독 또는 혼합물의 추출물로 이루어진 비만억제용 약제 등이 개발되어 있다. In particular, Cocis semen , Sanos ( Dioscoreae rhizoma ), Gilkyung ( Platycodi radix ), Bellflower, Schizandrae fructus , Citrus unshiu Markovich , Aloe vera and Adenophorae radix Some anti-obesity drugs have been developed, which consist of extracts of several herbal drugs or mixtures.
그러나 이제까지 알려진 이러한 천연소재 유래의 제품의 경우, 그 소재가 귀하여 매우 고가이거나, 적절한 효과를 얻기 위해 많은 양을 섭취해야 하거나, 실제 비만억제 및 고지혈증 방지를 위한 효과가 미미한 경우가 많았다.However, in the case of products derived from such natural materials so far known, the materials are very expensive, and in order to obtain a proper effect, they have to be consumed in large quantities, or the effects of preventing obesity and preventing hyperlipidemia are often insignificant.
따라서, 천연소재이면서도 입수가 용이하고, 보다 복합적인 효과를 나타낼 수 있는 새로운 생약 조성물을 연구 개발할 필요성이 있다.Therefore, there is a need to research and develop a new herbal composition that can be easily obtained even though it is a natural material and can have a more complex effect.
이에 본 발명자들은 종래 직간접적으로 당분의 소화흡수, 당분의 대사, 지질의 대사 등에 영향을 미치는 것으로 알려진 많은 전통 생약들을 예의 검토ㆍ분석하여 가장 우수한 비만억제 및 고지혈증 예방 효과를 나타내는 생약성분의 조합과 그들의 조성비를 찾아내게 되었다.Accordingly, the present inventors have studied and analyzed many traditional herbal medicines known to directly affect the digestion, sugar metabolism, lipid metabolism, and the like, directly and indirectly, and the combination of herbal ingredients showing the best anti-obesity and hyperlipidemic effect. I found their grant.
따라서 본 발명은 저렴하고 입수가 용이하며, 효과가 우수한 생약들의 최적 조합과 최적 조성비를 제시하여 우수한 비만억제 효과를 나타내는 조성물을 제공하는 것을 목적으로 한다.Therefore, an object of the present invention is to provide a composition exhibiting an excellent anti-obesity effect by presenting an optimal combination and optimal composition ratio of herbal medicines that are inexpensive and easy to obtain, and excellent in effectiveness.
또한 본 발명은 상기 비만억제용 조성물을 함유하는 약제 및 식품을 제공하는 것을 또 다른 목적으로 한다.It is another object of the present invention to provide a drug and a food containing the composition for inhibiting obesity.
즉, 본 발명의 목적은 비만증 및 이와 관련된 질환을 효율적으로 예방 및 억제할 수 있는 조성물을 제공하는 것이다.
That is, an object of the present invention is to provide a composition that can effectively prevent and suppress obesity and related diseases.
전술한 바와 같은 목적을 달성하기 위한 본 발명은, 길경(Platycodi radix) 추출물 1.0 중량부, 귤피(Citrus unshiu Markovich) 추출물 0.8~1.2 중량부, 백모근(Imperatae rhizoma) 추출물 1.4~3.5 중량부 및 맥문동(Liriopsis tuber) 추출물 1.1~1.7 중량부의 혼합물을 함유하는 비만억제 및 비만치료용 생약 조성물에 관한 것이다.The present invention for achieving the object as described above, 1.0 part by weight of Platycodi radix extract, 0.8 to 1.2 parts by weight of Citrus unshiu Markovich extract, 1.4 to 3.5 parts by weight of the imperae rhizoma extract and pulmonary sinus ( Liriopsis tuber ) extract relates to an herbal composition for inhibiting obesity and containing obesity containing 1.1 to 1.7 parts by weight of a mixture.
본 발명자들은 많은 실험과 검토 결과, 상기와 같은 함량비가 되어야 가장 양호한 생약 조성물이 얻어짐을 확인하였다.As a result of many experiments and studies, the present inventors have confirmed that the best herbal composition is obtained only with the above content ratio.
본 발명에 의한 상기 생약 조성물은 아래 실시예 및 적용예에서 볼 수 있듯이, 종래의 다른 생약 또는 시판중인 화학합성 비만억제 의약품에 비해 월등히 우수하고 안전한 비만억제 효과를 나타낸다.The herbal composition according to the present invention exhibits an excellent anti-obesity and safe anti-obesity effect as compared to other conventional herbal or commercial chemical synthetic anti-obesity medicines as shown in the following Examples and Applications.
본 발명에 의한 상기 생약 조성물은, 먼저 통상의 방법에 따라 각 조성물이 되는 생약을 각각 냉수추출, 열수추출 또는 용매추출 등의 방법으로 수득하고 건조한 다음, 상기 비율로 혼합하여 제조될 수 있다. 이 경우, 상기 각 생약은 서로 다른 방법으로 추출될 수도 있을 것이다. 예를 들면, 다음과 같은 방법으로 제조될 수 있다. 먼저, 선별되고 적절한 크기로 다듬어진 건조 길경, 귤피, 백모근 및 맥문동을 준비한다. 생약에 적절한 양의 순수를 가하고 100℃에서 3시간 열수추출을 행한 다음 영하 40℃에서 10-20시간 급속동결하고, 0.23토르 이하의 압력에서 35시간 이상 진공건조한 다음 분쇄하여 건조 분말을 준비한다. 이어서 각 생약의 건조분말을 상기 비율에 따라 혼합하여 본 발명에 의한 생약 조성물 분말을 수득한다. 물론, 건조되기 전의 각 생약 추출물의 고형물 함량을 사전에 조사한 다음 상기 비율이 되도록 추출물을 혼합한 다음 일괄적으로 건조하여 본 발명에 의한 생약 조성물 분말을 얻을 수도 있다. The herbal composition according to the present invention may be prepared by first obtaining a herbal medicine each of the compositions according to a conventional method by cold water extraction, hot water extraction or solvent extraction, drying, and then mixing in the above ratios. In this case, each herbal may be extracted in different ways. For example, it can be manufactured by the following method. First, prepare dried gilyeong, tangerine, white hairy root and pulsatile sinus, which have been screened and trimmed to an appropriate size. A suitable amount of pure water is added to the herbal medicine, hot water extraction is performed at 100 ° C. for 3 hours, and then rapidly frozen at minus 40 ° C. for 10-20 hours, vacuum dried at a pressure of 0.23 Torr or less for 35 hours, and then ground to prepare a dry powder. Subsequently, the dry powder of each herbal medicine is mixed by the said ratio, and the herbal composition powder which concerns on this invention is obtained. Of course, the solids content of each herbal extract before drying may be investigated in advance, and then the extracts may be mixed so as to have the above ratio and then dried in a batch to obtain the herbal composition powder according to the present invention.
한편, 본 발명에 의한 상기 생약 조성물은, 최종적으로 상기 비율이 될 수 있도록 계산된 비율의 각 생약 건조물을 먼저 혼합한 다음 일괄적으로 추출하여 수득되는 것도 가능하다. 이를 위하여, 건조 길경 1.0 중량부, 건조 귤피 0.8~1.2 중량부, 건조 백모근 2.3~3.5 중량부 및 건조 맥문동 0.8~1.2 중량부의 혼합물을 통상의 방법에 따라 냉수추출, 열수추출 또는 용매추출 등의 방법으로 각 성분의 혼합물을 추출한 다음, 여과하여 그대로 사용하거나, 농축하여 사용하거나, 동결건조하여 분말상으로 사용할 수 있다. 예를 들면, 다음과 같은 방법으로 제조될 수 있다. 먼저, 선별되고 적절한 크기로 다듬어진 건조 길경, 귤피, 백모근 및 맥문동을 상기 혼합비율에 맞추어 혼합한다. 혼합물에 적절한 양의 순수를 가하고 100 ℃에서 3시간 열수추출을 행한 다음 영하 40℃에서 10-20시간 급속동결하고, 0.23토르 이하의 압력에서 35시간 이상 진공건조한 다음 분쇄하여 본 발명에 의한 생약 조성물 분말을 수득한다.On the other hand, the herbal composition according to the present invention may be obtained by first mixing each herbal dry matter of the calculated ratio so as to finally be the ratio and then extracted in a batch. To this end, a mixture of 1.0 parts by weight of dry path length, 0.8 to 1.2 parts by weight of dried tangerine, 2.3 to 3.5 parts by weight of dried white hair root and 0.8 to 1.2 parts by weight of dried Macmundong according to a conventional method, such as cold water extraction, hot water extraction or solvent extraction The mixture of each component is extracted, and then filtered and used as it is, or used by concentration, or lyophilized to be used as a powder. For example, it can be manufactured by the following method. First, the selected dried and cured gilyeong, tangerine, white hair root and pulmonary dong are appropriately mixed to the mixing ratio. The crude drug composition according to the present invention is added to the mixture with an appropriate amount of pure water, followed by hot water extraction at 100 ° C. for 3 hours, then rapidly freezing at 40 ° C. for 10-20 hours, vacuum drying at a pressure of 0.23 Torr or less for 35 hours, and then pulverizing. Obtain a powder.
본 발명은 또한 상기 생약 조성물을 유효성분으로 함유하는 비만치료ㆍ억제용 약제 및 건강기능식품에 관한 것이다. 상기 비만치료ㆍ억제용 약제 및 건강기능식품에는, 상기 생약 조성물 이외에 필요에 따라 다양한 보조 생약제, 비타민, 미네랄, 식이섬유 및 기타 의약용-식품용 보조제(예컨대, 부형제, 증강제, 코팅제 등)등이 함유될 수 있을 것이다.The present invention also relates to a medicament for obesity treatment and suppression and a health functional food containing the herbal composition as an active ingredient. In addition to the herbal composition, various supplemental herbal medicines, vitamins, minerals, dietary fiber and other medicinal-food supplements (e.g., excipients, enhancers, coatings, etc.) may be used for the obesity treatment / inhibitory agent and health functional food. It may be contained.
본 발명은 또한 상기 생약 조성물을 유효성분으로 함유하면서, 세포내 β3AR 활성을 증가시키는 약제학적 조성물에 관한 것이다. 상기 약제학적 조성물에도 역시 필요에 따라 다양한 보조 생약제, 비타민, 미네랄, 식이섬유 및 기타 의약용-식품용 보조제(예컨대, 부형제, 증강제, 코팅제 등)등이 함유될 수 있을 것이다.The present invention also relates to a pharmaceutical composition which increases the intracellular β3AR activity while containing the herbal composition as an active ingredient. The pharmaceutical composition may also contain various supplemental herbal medicines, vitamins, minerals, dietary fiber and other medicinal-food supplements (eg, excipients, enhancers, coatings, etc.) as needed.
이하 본 발명을 실시예 및 적용예에서 보다 상세하게 설명한다. 하기 실시예는 본 발명을 보다 상세히 설명하고자하는 예시적인 것일 뿐 이에 의해 본 발명의 기술적 사상의 본질이 변하거나 범위가 축소되는 것은 아니다. 하기 실시예에서 제시되지 않은 여러 가지 실시예 및 적용예 들이 가능함은 당업자에게 있어 당연할 것이다.Hereinafter, the present invention will be described in more detail in Examples and Application Examples. The following examples are merely illustrative of the present invention in detail, and thus, the nature of the technical idea of the present invention is not changed or reduced in scope. It will be apparent to those skilled in the art that various embodiments and applications not shown in the following examples are possible.
실시예 : 본 발명에 의한 생약 조성물의 제조Example: Preparation of herbal composition according to the present invention
(1) 미리 선별하여 적절한 크기로 절단한 각각 5 Kg의 건조 길경, 귤피, 백모근 및 맥문동에 10배 중량의 물을 혼합한 다음 가열하여 100℃에서 3시간 동안 열수추출을 행하였다. 이어서 영하 40℃에서 15시간 급속동결하고, 0.23토르 이하의 압력하에서 35시간 이상 진공건조한 다음 분쇄하여 각각의 건조분말을 수득하였다. (1) 10 times weight of water was mixed in each of 5 Kg of dried Kilkyung, Kalpipi, White Hairy root and Macmundong, which were previously screened and cut to an appropriate size, followed by heating and performing hot water extraction at 100 ° C. for 3 hours. Subsequently, rapid freezing was carried out at minus 40 ° C. for 15 hours, vacuum dried for at least 35 hours under a pressure of 0.23 Torr or less, and then ground to obtain respective dry powders.
수득된 길경, 귤피, 백모근 및 맥문동 추출 건조분말을 1:1:1.8:1.4의 비율로 혼합하여 본 발명의 생약 조성물 분말을 수득하였다.The obtained gilyeong, tangerine peel, white hair root and pulmonary pulverized extract powder were mixed in a ratio of 1: 1: 1.8: 1.4 to obtain the herbal composition powder of the present invention.
(2) 미리 상기 각 생약의 추출효율을 분석한 다음 최종 추출물에서 각 성분의 비율이 길경:귤피:백모근:맥문동 =1:1:1.8:1.4 가 되도록 각 건조 생약을 혼합하였다. 즉, 미리 선별하여 적절한 크기로 절단되어 있는 건조 길경 1kg, 귤피 1kg, 백모근 2.9kg 및 맥문동 1kg을 혼합하고 10배 중량의 물을 부은 다음 가열하여 100℃에서 3시간 동안 열수추출을 행하였다. 이어서 영하 40℃에서 15시간 급속동결하고, 0.23토르 이하의 압력하에서 35시간 이상 진공건조한 다음 분쇄하여 본 발명의 생약 조성물 분말 0.83kg을 수득하였다.(2) The extraction efficiency of each herbal medicine was analyzed in advance, and then each dried herbal medicine was mixed so that the ratio of each component in the final extract was Gilkyung: Gangpi: White hair root: Mangmun-dong = 1: 1: 1.8: 1.4. In other words, 1kg of dry length, 1kg, tangerine peel 1kg, white hair root 2.9kg, and 1kg of gingimun dong, which were selected and cut in advance, were mixed, poured with 10 times the weight of water, and heated to extract hot water at 100 ° C. for 3 hours. Subsequently, the solution was rapidly frozen at 40 ° C. for 15 hours, vacuum-dried at least 35 hours under a pressure of 0.23 Torr or less, and then ground to obtain 0.83 kg of the herbal composition powder of the present invention.
(3) 여러 in vitro, in vivo 실험 결과(데이터 도시 생략), 상기 2가지 방법으로 제조된 본 발명에 의한 생약 조성물은 동일물로 확인되었다. 따라서 이하 실험에서는 2가지 방법에 의한 것을 구별하지 않고 적용예에 이용하였다.(3) Results of various in vitro and in vivo experiments (not shown in the data), the herbal compositions according to the present invention prepared by the above two methods were identified as the same. Therefore, in the following experiment, it used for the application example, not distinguishing by the two methods.
적용예 1 : 3T3L1 cell을 이용한 in vitro 실험을 통한 본 발명에 의한 조성물의 효과 분석Application Example 1: Analysis of the effect of the composition according to the invention through in vitro experiments using 3T3L1 cell
β3AR(β-3-adrenergic receptor)은 지방 세포에서 주로 발현되며 지방 분해와 열 발산 과정에 관여하는 유전자로 잘 알려져 있다. 예를 들어 이 유전자가 소실된 생쥐의 경우, 일반 식이에서 정상 생쥐에 비해 물질 대사율의 감소로 약간의 비만을 보이고, 지방 식이에서는 비만도가 크게 증가함이 보고 된 바 있다 (Bachman, E. S, Science 297: 843-845, 2002). 또한 정상인과 비만인을 대상으로 한 일본 연구에서 β3AR의 유전자 돌연변이에 따라 복부 비만도에 차이가 있음이 보고 된 바 있다(Kim-Motoyama, Diabetologia 40: 469-472, 1997). 이는 이 유전자의 소실 또는 기능 저하로 지방 식이에 따른 지방 분해와 열 발산이 억제되어 나타나는 결과이다. β-3-AR (β-3-adrenergic receptor) is mainly expressed in fat cells and is well known as a gene involved in the process of lipolysis and heat dissipation. For example, mice that have lost this gene have been shown to have a slight obesity due to a decrease in metabolism in normal diets and a significant increase in obesity in fat diets (Bachman, E. S, Science 297: 843-845, 2002). In addition, Japanese studies on normal and obese people have reported differences in abdominal obesity according to β3AR gene mutations (Kim-Motoyama, Diabetologia 40: 469-472, 1997). This is a result of the loss or function of this gene, resulting in suppressed fat breakdown and heat dissipation due to fat diet.
이에 따라 본 적용예에서는 각종 약제 처리군이 비만조절에 관여하는 β3AR의 발현에 미치는 효과를 분석하였다. Accordingly, in this application example, the effect of various drug treatment groups on the expression of β3AR involved in obesity control was analyzed.
사전에 통상의 방법으로 미분화 지방세포(pre-adipocyte)인 3T3L1세포를 약 2×106 cell/㎖의 농도가 되도록 배양한 다음, 인슐린(Insulin)과 인도메타신( Indomathasin )을 처리하여 지방세포(adipocyte)로 분화시킨 후, 세포배양액 1㎖ 당 본 발명에 의한 생약 조성물과 현재 비만억제제로 시판되고 있는 리덕틸R(Sibutramine HCL,일성신약) 및 본 생약 조성물의 구성성분 각각 즉, 귤피, 길경, 맥문동 및 백모근 추출물(생약들은 본 발명에 의한 조성물 수득방법과 동일 한 방법으로 수득)을 각각 10, 100, 200 ㎍ 씩 처리하여 37℃에서 24시간 배양한 후, 세포로부터 mRNA를 추출하였다. 추출한 mRNA를 동일량으로 역전사 중합효소연쇄반응(reverse transcription - polymerase chain reaction) 을 이용하여 β3AR의 발현도(도 1 : PCR 산물의 전기영동 사진 위의 것)를 조사하였다. 또한 각 처리군 당 동일량의 총 mRNA가 존재함을 볼 수 있는 내부 대조군(internal control)인 베타-액틴(β-actin)의 발현도를 함께 조사하였다(도 1 : PCR 산물의 전기영동 사진 아래의 것). 베타-액틴은 세포에서 동일한 정도로 발현됨을 보기위해 보편적으로 사용되는 유전자로, 각 처리군에 총 mRNA량이 동일하게 존재함을 보기 위해 측정한 것이다. In a conventional manner, 3T3L1 cells, which are pre-adipocytes, are cultured to a concentration of about 2 × 10 6 cells / ml, and then treated with insulin (Insulin) and indomethasin (Indomathasin) to adipocytes. After differentiation into (adipocyte), each medicinal herb composition according to the present invention per 1ml of cell culture medium and the components of the medicinal composition, ie, ductilum, gilyeong, Megmundong and white hair root extracts (medicines obtained in the same manner as the method of obtaining a composition according to the present invention) were treated with 10, 100 and 200 ㎍, respectively, and cultured at 37 ° C for 24 hours, and then mRNA was extracted from the cells. The expression level of β3AR (FIG. 1: above the electrophoretic image of the PCR product) was investigated by using reverse transcription-polymerase chain reaction. In addition, the expression level of beta-actin (β-actin), which is an internal control that shows the presence of the same amount of total mRNA in each treatment group, was examined together (Fig. 1: electrophoresis picture of PCR product) that). Beta-actin is a gene that is commonly used to see the same level of expression in cells and is measured to see that the total amount of mRNA is the same in each treatment group.
상기에서 언급하였듯이 비만은 여러 기전을 통해 지방세포에 지방이 축적되는 것으로 알고 있으므로 이에 근거하여 미분화 지방세포인 3T3L1에 인슐린과 인도메타신을 처리하여 지방세포로 분화시키는 in vitro 세포 시스템을 이용하여 본 발명 “조성물”이 β3AR의 발현도에 미치는 효과를 본 것이다.As mentioned above, since obesity is known to accumulate fat in adipocytes through various mechanisms, the present invention uses an in vitro cell system that differentiates into adipocytes by treating insulin and indomethacin to undifferentiated adipocytes 3T3L1. We have seen the effect of "composition" on the expression level of β3AR.
도 1의 a에서, 위는 β3AR, 아래는 베타-액틴(β-actin)의 PCR 산물의 전기영동 사진이며, 도 1의 b는 해당 레인의 강도(intensity)를 정량 값으로 표시한 것이다. 도 1의 사진과 도표에서 볼 수 있듯이, 본원 발명에 의한 생약 조성물을 200, 100, 10ug/ml 처리한 경우, 비만 조절에 중요한 역할을 하는 β3AR에 대한 발현도가 시판중인 비만억제제인 리덕틸 보다 약 2배 정도 높았으며, 귤피나 백모근 단일 처리군에서 보다 좋은 발현효과를 나타내었다. 도1a 아래 그림에서 볼 수 있듯이, 모든 처리군에서 베타-액틴(β-actin)의 발현량에는 유의할 만한 차이가 없었다. 이는, 동일한 양의 총 mRNA에 대해 약제 처리군 별로 β3AR의 발현 차가 있음을 의미하며, 그러므로 각 처리군 효과 차이는 총 mRNA의 차이가 아니라, β3AR 특정 유전자의 mRNA 발현 차이에 의한 것임을 알 수 있었다.In Figure 1a, the top is β3AR, the bottom is an electrophoretic picture of the PCR product of beta-actin (β-actin), Figure 1b is the intensity (intensity) of the lanes as a quantitative value. As can be seen in the photos and diagrams of Figure 1, 200, 100, 10ug / ml of the herbal composition according to the present invention, the expression level for β3AR that plays an important role in the control of obesity is about 2 than the commercially available obesity inhibitor reductil It was about twice as high, and showed better expression effect in single treatment group of Kippi or white hair root. 1a As can be seen in the figure below, there was no significant difference in the expression level of beta-actin (β-actin) in all treatment groups. This means that there is a difference in the expression of β3AR for each drug treatment group for the same amount of total mRNA. Therefore, the difference in effect of each treatment group was not due to the difference in the total mRNA, but was due to the mRNA expression difference of the β3AR specific gene.
따라서 본 발명에 의한 비만억제용 생약 조성물은 종래 여타 화학합성 제품이나 단일 생약재에 비해 우수한 비만억제 효과를 보임을 확인할 수 있었다. Therefore, it was confirmed that the herbal composition for inhibiting obesity according to the present invention showed superior anti-obesity effect compared to other chemical synthesis products or single herbal medicines.
적용예 2 : 본 발명에 의한 조성물의 체중감량 및 지혈증 개선 효과 분석 1Application Example 2 Analysis of the weight loss and hemostatic improvement effect of the composition according to the present invention 1
(1) 총 35마리의 c57BL/6 생쥐를 대조군 10 마리와 본 발명에 의한 생약 조성물 투여군 10 마리, 리덕틸 투여군 6 마리, 국내 유명 다이어트 식품인 진슬림 다이어트 투여군 5 마리 등 4개의 군으로 나누어 4 주간 고지방 식이(Diet #101556ccl, Dyets Inc., U.S.)를 급여하면서 하루 1회 체중 kg 당 600mg 씩 경구 투여하였다. 그 후 4 주간은 투여량을 kg 당 1g으로 증가시키고 체중 변화량을 측정하였다. 결과는 표 1에 나타내었다.(1) A total of 35 c57BL / 6 mice were divided into four groups: 10 control groups, 10 herbal drug administration groups according to the present invention, 6 reductil-administered groups, and 5 Ginslim diet-administered groups, which are well-known domestic diet foods, for 4 weeks. A high fat diet (Diet # 101556ccl, Dyets Inc., US) was administered orally 600 mg / kg body weight once daily. Four weeks thereafter the dose was increased to 1 g / kg and body weight change was measured. The results are shown in Table 1.
표1에서 볼 수 있듯이, 투여 초기 4 주 동안에는 본 발명에 의한 조성물 투여군이 합성 약제인 리덕틸 투여군 보다 체중 증가량이 다소 증가하였으나, 후기 4 주 투여기간 동안에는 오히려 평균 체중이 감소되는 효과를 나타내었다. 리덕틸의 경우도 평균 0.3g 증가로 그 증가가 미미하긴 하였으나, 최소값과 최대값 사이의 간격이 매우 큰(따라서 표준편차가 매우 큰) 현상을 나타내었다. 표준편차가 크다는 것은 개체마다 약효가 달리 나타나며, 약효의 유의성이 적다는 것을 의미한다.As can be seen in Table 1, during the first four weeks of administration, the composition-administered group according to the present invention slightly increased the weight gain than the synthetic drug reductil-administered group, but the average weight was decreased during the later four-week administration period. In the case of reductil, the average increase was 0.3g, but the increase was small, but the gap between the minimum value and the maximum value was very large (and therefore the standard deviation was very large). A large standard deviation means that the drug is different for each individual and that the drug is less significant.
본 발명에 의한 조성물을 투여한 경우, 다른 화학합성 비만 억제제나 비만 억제용 건강식품을 투여한 경우에 비해 평균 체중 감소효과가 월등히 뛰어나면서도 그 효과가 고르게 나타나고 있음(즉, 체중 최소 증가량과 최대 증가량 간격이 좁다는 의미 = 체중증감에 대한 표준편차 값이 적다는 의미)을 확인할 수 있었다.In the case of administering the composition according to the present invention, the average weight loss effect is superior to that in the case of administration of other chemical synthesis obesity inhibitors or obesity inhibitory health foods, but the effect is shown evenly (that is, the minimum and maximum weight gains) Meaning that the interval is narrow = means that the standard deviation value for weight change is small).
(2) 전술한 (1)의 실험과정에서 실험 8주 경과 후, 각 마우스의 혈액을 채취하여 혈청검사를 수행하였다(표 2)(2) Eight weeks after the experiment in the above-described experiment (1), blood of each mouse was collected and serologically performed (Table 2).
표2에서 볼 수 있듯이, 본 발명에 의한 조성물 투여군의 경우, 거의 모든 혈액관련 수치가 다른 투여군에 비해 우수함을 알 수 있다. 특히 총 콜레스테롤 함량이 다른 투여군 보다 낮으면서도 유용한 콜레스테롤인 HDL-콜레스테롤의 비율이 높게 나타났다.As can be seen in Table 2, in the case of the composition administration group according to the present invention, it can be seen that almost all blood-related values are superior to other administration groups. In particular, the ratio of HDL-cholesterol, a useful cholesterol, was lower than that of other administration groups.
이에 의해, 본 발명에 의한 생약 조성물은 고지혈증의 예방 및 치료에도 유용하게 적용될 수 있음을 확인할 수 있었다.Thereby, it was confirmed that the herbal composition according to the present invention can be usefully applied to the prevention and treatment of hyperlipidemia.
적용예 3 : 본 발명에 의한 조성물의 체중감량 및 지혈증 개선 효과 분석 2Application Example 3 Analysis of the weight loss and hemostatic improvement effect of the composition according to the present invention 2
(1) 질환동물 모델 DB/DB mouse를 23 마리를 대조군 7 마리와 본 발명에 의한 생약 조성물 투여군 6 마리, 리덕틸 투여군 6 마리, 진슬림 다이어트 투여군 6 마리로 나누어 삼양배합사료(마우스용)를 투여하면서 전기 적용예 2의 (1)에서와 같은 방법으로 사료들을 경구투여하고, 동일한 방법으로 군별 체중 증가량을 분석하였다(표 3).(1) The disease animal model DB / DB mouse is divided into seven control groups and six herbal composition administration groups according to the present invention, six reductyl administration groups, six Ginslim diet administration groups, and six Samyang compound feeds (for mice). While the feeds were orally administered in the same manner as in the above (1) of Application Example 2, the weight gain of each group was analyzed by the same method (Table 3).
표3에서 볼 수 있듯이, 질환동물을 모델로 한 본 적용예에서도 전기 적용예 2에서와 동일한 결과가 나타났다. 즉, 본 발명에 의한 조성물 투여군의 경우, 타 약제 투여군에 비해 체중 증가량이 적거나 감소하면서도 표준편차가 비교적 적게 나타났다. 이로서 본 발명에 의한 조성물은 비만 질환자의 치료에도 효과가 있음을 확인할 수 있었다.As can be seen in Table 3, the same results as in the previous application example 2 also appeared in this application model of the diseased animal. That is, in the case of the composition administration group according to the present invention, the amount of weight gain was decreased or decreased, but the standard deviation was relatively smaller than that of the other drug administration group. As a result, the composition according to the present invention was confirmed to be effective in the treatment of obese patients.
(2) 비만생쥐에서는 시상하부(hipothalamus)에 NPY (neuropeptide Y)의 농도가 증가되어 중추신경을 자극하고, 식이섭취와 인슐린 분비를 증가시켜 WAT (white adipocyte tissue)에서의 비만유전자 발현을 증가시키게 된다. 이는 인슐린이 WAT에서 비만유전자를 up- and down- regulation하는 생리적인 역할을 할 수 있어 adipocytes에 triglyceride의 축적과 leptin 분비를 자극하여 복강내 adipocytes의 증식과 WAT의 증가를 초래한다. 또한 비만생쥐에서 과다한 식이섭취와 호르몬 분비는 간세포들의 증식과 활성화로 혈중 glucose, cholesterol, 그리고 triglyceride 단백질을 증가시켜 간기능 장애를 초래한다. 이러한 간기능의 장애는 GPT, GOT, 그리고 creatinine의 증가를 가져오고, 과잉대사작용에 대한 feedback이 억제되어 비만의 정도가 계속적으로 증가하게 된다 (Meinders, A.E , A.C. Toornvliet, H. Pijl. Leptin, Netherlands journal of medicine 49 (1996) 247-252). (2) In obese mice, the concentration of NPY (neuropeptide Y) is increased in the hypothalamus, which stimulates the central nervous system, increases dietary intake and insulin secretion, and increases the expression of obesity genes in white adipocyte tissue (WAT). do. Insulin plays a physiological role in up- and down-regulation of obesity genes in WAT, which stimulates triglyceride accumulation and leptin secretion in adipocytes, leading to proliferation of adipocytes in the abdominal cavity and an increase in WAT. Excessive dietary intake and hormone secretion in obese mice lead to hepatic dysfunction by increasing blood glucose, cholesterol, and triglyceride proteins due to the proliferation and activation of hepatocytes. This impairment of liver function leads to an increase in GPT, GOT, and creatinine, and the suppression of overmetabolism is suppressed and the degree of obesity continues to increase (Meinders, AE, AC Toornvliet, H. Pijl. Leptin, Netherlands journal of medicine 49 (1996) 247-252).
이와 관련하여 전술한 (1)의 실험과정에서 실험 8주 경과 후, 각 마우스의 혈액을 채취하여 혈청검사를 수행하였다(표 4 참조)In this regard, after eight weeks of the experiment in the above-described experiment (1), blood of each mouse was collected and serologically performed (see Table 4).
표4에서 볼 수 있듯이, 대조군의 비만생쥐에서 GOT, GPT, Glucose, 그리고 creatinine이 크게 증가되었으나, 본 발명에 의한 조성물 투여군에서 현저히 감소되는 것을 확인할 수 있었다. 그리고 adipocytes의 활성화로 대조군에서 insulin 과 leptin의 분비량이 증가한 반면, 조성물 투여로 비만유전자의 발현이 조절되어 insulin과 leptin의 분비가 현저히 감소됨을 알 수 있었다.As shown in Table 4, GOT, GPT, Glucose, and creatinine were significantly increased in obese mice of the control group, but it was confirmed that the composition administration group according to the present invention is significantly reduced. The activation of adipocytes increased the secretion of insulin and leptin in the control group, whereas the expression of the obesity gene was regulated by the administration of the composition, resulting in a significant decrease in insulin and leptin secretion.
또한 본 발명에 의한 조성물을 투여한 군은 혈청검사 수치가 대조군뿐만 아니라 다른 화학합성 비만치료제에 비해 전체적으로 우수한 결과를 나타내었다.In addition, the group administered with the composition according to the present invention showed an excellent overall serum test results compared to the control group as well as other chemotherapy drugs.
즉, 본 발명에 의한 조성물 투여군에서는 비만 및 당뇨와 깊은 연관이 있는 혈중 포도당(glucose) 수치 및 인슐린(insulin) 수치가 리덕틸과 유사함을 보여주고 있다. 한편, 본 발명의 조성물 처리군에서 크레아티닌의 수치가 대조군과 비슷한데, 이는 본 발명의 조성물이 신장(kidney)에 특이적인 부담을 주지 아니한다는 것을 확인하는 것이다.That is, the composition administration group according to the present invention shows that blood glucose levels and insulin levels closely related to obesity and diabetes are similar to reductyl. On the other hand, the level of creatinine in the composition treatment group of the present invention is similar to the control group, which confirms that the composition of the present invention does not place a specific burden on the kidney (kidney).
결론적으로, 본 발명에 의한 조성물 투여군의 경우, 거의 모든 혈액관련 수치가 다른 투여군에 비해 우수함을 알 수 있다. In conclusion, in the case of the composition administration group according to the present invention, it can be seen that almost all blood-related values are superior to other administration groups.
이에 의해, 본 발명에 의한 생약 조성물은 비만과 연관된 질병의 치료 및 예방에 유용하게 적용될 수 있음을 확인할 수 있었다.Accordingly, it was confirmed that the herbal composition according to the present invention can be usefully applied to the treatment and prevention of diseases associated with obesity.
이상에서 검토한 바와 같이, 본 발명에 의한 생약 조성물은 세포에서 비만예방 및 비만치료에 관련된 유전자의 발현을 촉진시키며, 고 지방 식이를 투여한 마우스의 경우 매우 우수한 체중증가 억제효과 및 혈액 중 지방의 양 및 조성을 개선시켜서, 비만질병 마우스에 투여하는 경우에도 우수한 효과를 나타낸다.As discussed above, the herbal composition according to the present invention promotes the expression of genes related to the prevention of obesity and the treatment of obesity in cells. The amount and composition are improved to show an excellent effect even when administered to obese mice.
본 발명에 의한 생약 조성물을 비만억제 및 비만치료용 약제 또는 건강기능 식품의 유효성분으로 활용하는 경우, 천연의 성분이 적용된 것이므로 사용자의 거부감을 없앨 수 있으며, 비만억제에 따른 다른 신체부위 및 장기에 부정적인 영향이 없는 우수한 제품의 제공이 가능하게 된다.When the herbal composition according to the present invention is used as an active ingredient of an obesity inhibitor and an anti-obesity agent or a health functional food, natural ingredients are applied so that the user's rejection can be eliminated and other body parts and organs caused by obesity inhibition It is possible to provide excellent products without negative effects.
Claims (6)
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| KR20050078601A KR20050078601A (en) | 2005-08-05 |
| KR100573590B1 true KR100573590B1 (en) | 2006-04-24 |
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| KR1020040006785A KR100573590B1 (en) | 2004-02-02 | 2004-02-02 | New Herbal Composition for Treatment and Prevention of Obesity |
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Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
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| KR20200135621A (en) | 2019-05-23 | 2020-12-03 | 주식회사 하람 | Obesity prevention and treatment materials with Quercetin-3-O-glucuronide as a valid ingredient |
Families Citing this family (1)
| Publication number | Priority date | Publication date | Assignee | Title |
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| KR101511364B1 (en) * | 2008-04-29 | 2015-04-10 | 주식회사 유유제약 | Herbal Extract Composition for Prevention or Treatment of Obesity and Metabolic Syndrome Using Herbal Extract |
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Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| KR20200135621A (en) | 2019-05-23 | 2020-12-03 | 주식회사 하람 | Obesity prevention and treatment materials with Quercetin-3-O-glucuronide as a valid ingredient |
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| Publication number | Publication date |
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| KR20050078601A (en) | 2005-08-05 |
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