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Hepatic STAMP2 decreases hepatitis B virus X protein-associated metabolic deregulation
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  • Hepatic STAMP2 decreases hepatitis B virus X protein-associated metabolic deregulation
  • Hepatic STAMP2 decreases hepatitis B virus X protein-associated metabolic deregulation
저자명
Kim. Hye Young,Cho. Hyun Kook,Yoo. Seong Keun,Cheong. JaeHun
간행물명
Experimental & molecular medicine : EMM
권/호정보
2012년|44권 10호|pp.622-632 (11 pages)
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생화학분자생물학회
파일정보
정기간행물|ENG|
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이 논문은 한국과학기술정보연구원과 논문 연계를 통해 무료로 제공되는 원문입니다.
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기타언어초록

Six transmembrane protein of prostate 2 (STAMP2) plays a key role in linking inflammatory and diet-derived signals to systemic metabolism. STAMP2 is induced by nutrients/feeding as well as by cytokines such as $TNF{alpha}$, IL-$1{eta}$, and IL-6. Here, we demonstrated that STAMP2 protein physically interacts with and decreases the stability of hepatitis B virus X protein (HBx), thereby counteracting HBx-induced hepatic lipid accumulation and insulin resistance. STAMP2 suppressed the HBx-mediated transcription of lipogenic and adipogenic genes. Furthermore, STAMP2 prevented HBx-induced degradation of IRS1 protein, which mediates hepatic insulin signaling, as well as restored insulin-mediated inhibition of gluconeogenic enzyme expression, which are gluconeogenic genes. We also demonstrated reciprocal expression of HBx and STAMP2 in HBx transgenic mice. These results suggest that hepatic STAMP2 antagonizes HBx-mediated hepatocyte dysfunction, thereby protecting hepatocytes from HBV gene expression.