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Equol inhibits prostate cancer growth through degradation of androgen receptor by S‐phase kinase‐associated protein 2
Authors:Momoe Itsumi  Masaki Shiota  Ario Takeuchi  Eiji Kashiwagi  Junichi Inokuchi  Katsunori Tatsugami  Shunichi Kajioka  Takeshi Uchiumi  Seiji Naito  Masatoshi Eto  Akira Yokomizo
Affiliation:1. Department of Urology, Graduate School of Medical Sciences, Kyushu University, Fukuoka, Japan;2. Department of Clinical Chemistry and Laboratory Medicine, Graduate School of Medical Sciences, Kyushu University, Fukuoka, Japan;3. Department of Urology, Harasanshin Hospital, Fukuoka, Japan
Abstract:
Chemopreventive and potential therapeutic effects of soy isoflavones have been shown to be effective in numerous preclinical studies as well as clinical studies in prostate cancer. Although the inhibition of androgen receptor signaling has been supposed as one mechanism underlying their effects, the precise mechanism of androgen receptor inhibition remains unclear. Thus, this study aimed to clarify their mechanism. Among soy isoflavones, equol suppressed androgen receptor as well as prostate‐specific antigen expression most potently in androgen‐dependent LNCaP cells. However, the inhibitory effect on androgen receptor expression and activity was less prominent in castration‐resistant CxR and 22Rv1 cells. Consistently, cell proliferation was suppressed and cellular apoptosis was induced by equol in LNCaP cells, but less so in CxR and 22Rv1 cells. We revealed that the proteasome pathway through S‐phase kinase‐associated protein 2 (Skp2) was responsible for androgen receptor suppression. Taken together, soy isoflavones, especially equol, appear to be promising as chemopreventive and therapeutic agents for prostate cancer based on the fact that equol augments Skp2‐mediated androgen receptor degradation. Moreover, because Skp2 expression was indicated to be crucial for the effect of soy isoflavones, soy isoflavones may be applicable for precancerous and cancerous prostates.
Keywords:Androgen receptor  isoflavone  prostate cancer  prostate‐specific antigen  Skp2
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