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논문 기본 정보

자료유형
학술저널
저자정보
Munji Choi (성신여자대학교) Jinpyo An (경기대학교) Ae Jung Kim (경기대학교) Myoungsook Lee (성신여자대학교)
저널정보
동아시아식생활학회 동아시아식생활학회지 東아시아 食生活學會誌 第24卷 第3號
발행연도
2014.6
수록면
335 - 350 (16page)
DOI
10.17495/easdl.2014.06.24.3.335

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초록· 키워드

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Compared to the large numbers of studies on the diabetes, hyperlipidemia and cancer therpeutic effects of ginseng, the anti-obese effect and mechanisms of ginsengs have not been studied as much. To determine the effects of ginseng on obesity, 14 keywords (ginseng, ginsenoside, obesity, weight, fat, diet, overeat, appetite, lipid, 3T3-L1, adipocyte, food intake, adipogenesis and lipolysis) were combined in searching a database. Fifty-six articles published from 1983 to 2012 as well as 656 patents registered until Aug 17<SUP>th</SUP>, 2012, were screened for anti-obese effects of ginseng. In the classification of experimental methods, 16 papers on 3T3-L1 cells, 38 papers on animals and three papers on human were reviewed. In terms of obese mechanisms of action, the most commonly used biomarkers were in order of lipid profiles > weight change > blood glucose > adipocytokine. Most ginseng studies on obesity focused on AMPK, PPARγ, GLUT-4, PI3K and SREBP-1. Korean white ginseng extracts and Re repressed the lipogenesis genes such as PPARc2, SREBP-1c, LPL, FAS and DGAT1. However, ginseng or ginsenosides, PD (Rb1) and PT (Re), showed different or contradictory results. Water and ethanol extraction of ginseng showed contradictory effects on the secretion of inflammatory cytokines, wheras IL-6 was repressed by ethanol extracts and TNF-α repressed by Re in vitro. Based on the literature, further studies on anti-obese mechanisms of ginseng, such as the inflammation-related obesity or cross signals between the adipocytes and the environments, are needed, instead of more studies on its hypolipidemic and hypoglycemic effects.

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Abstracts
INTRODUCTION
SUBJECTS OF RESEARCH PAPERS AND PATENTS
IN VITRO STUDIES OF GINSENG ON ANTIOBESITY
IN VIVO STUDIES OF GINSENG ON ANTICBESITY
PERSPECTIVES
REFERENCES

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UCI(KEPA) : I410-ECN-0101-2015-590-001651436