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Research Frontiers
of Medicinal Plants
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人參達瑪烷皂苷Rh2的藥理作用簡述



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達瑪烷皂苷Rg1的藥理作用簡述



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達瑪烷皂苷Rb1的藥理作用簡述



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達瑪烷苷元原人參三醇PPT的藥理作用簡述



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達瑪烷苷元原人參二醇PPD的藥理作用簡述


 

達瑪烷皂苷元PPD(原人參二醇)誘導人黑色素瘤自殺

達瑪烷苷元PPD(原人參二醇)對肺癌的細胞與動物實驗研究
小細胞肺癌(Small Cell Lung Cancer,SCLC)約佔肺癌的20%,尤以吸煙人群為高發人群,小細胞肺癌患者中90%以上的人有吸煙史。小細胞肺癌的發病年齡35-68歲,平均發病年齡60歲,男性多於女性。小細胞肺癌早期可無症狀,因此發現時多為中晚期。 小細胞肺癌惡性程度高,倍增時間短,轉 ​​移早而廣泛,對化療、放療敏感,初治緩解率高。但是,小細胞費按極易發生繼發性耐藥,從而導致化療失效。 人參皂苷,尤其是原人參二醇組的皂苷的抗癌活性已逐漸被學界所認識。最近在中草藥(2008年...
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The Ginsenoside 20-O-β-D-Glucopyranosyl-20(S)-Protopanaxadiol Induces Autophagy and Apoptosis in Human Melanoma via AMPK/JNK Phosphorylation.
PLoS One. 2014;9(8):e104305
Authors: Kang S, Kim JE, Song NR, Jung SK, Lee MH, Park JS, Yeom MH, Bode AM, Dong Z, Lee KW

Abstract
Studies have shown that a major metabolite of the red ginseng ginsenoside Rb1, called 20-O-β-D-glucopyranosyl-20(S)-protopanaxadiol (GPD), exhibits anticancer properties. However, the chemotherapeutic effects and molecular mechanisms behind GPD action in human melanoma have not been previously investigated.

Here we report the anticancer activity of GPD and its mechanism of action in melanoma cells. GPD, but not its parent compound Rb1, inhibited melanoma cell proliferation in a dose-dependent manner.

Further investigation revealed that GPD treatment achieved this inhibition through the induction of autophagy and apoptosis, while Rb1 failed to show significant effect at the same concentrations.

The inhibitory effect of GPD appears to be mediated through the induction of AMPK and the subsequent attenuation of mTOR phosphorylation. In addition, GPD activated c-Jun by inducing JNK phosphorylation.

Our findings suggest that GPD suppresses melanoma growth by inducing autophagic cell death and apoptosis via AMPK/JNK pathway activation.

GPD therefore has the potential to be developed as a chemotherapeutic agent for the treatment of human melanoma.

PMID: 25137374 [PubMed - as supplied by publisher]

Source: PPT and PPD

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