激活素2型受体
卵泡抑素
ACVR2B型
癌变
激活素受体
生物
转化生长因子
肝细胞癌
癌症研究
转化生长因子β信号通路
六氯环己烷
转化生长因子β
细胞生物学
受体
肝癌
内分泌学
内科学
癌症
医学
遗传学
作者
Alev Deli,Emanuel Kreidl,Stefan Santifaller,Barbara Trotter,Katja Seir,Walter Berger,Rolf Schulte‐Hermann,Chantal Rodgarkia‐Dara,Michael Grusch
摘要
In many parts of the world hepatocellular carcinoma (HCC) is among the leading causes of cancer-related mortality but the underlying molecular pathology is still insufficiently understood. There is increasing evidence that activins, which are members of the transforming growth factor beta (TGFbeta) superfamily of growth and differentiation factors, could play important roles in liver carcinogenesis. Activins are disulphide-linked homo- or heterodimers formed from four different beta subunits termed betaA, betaB, betaC, and betaE, respectively. Activin A, the dimer of two betaA subunits, is critically involved in the regulation of cell growth, apoptosis, and tissue architecture in the liver, while the hepatic function of other activins is largely unexplored so far. Negative regulators of activin signals include antagonists in the extracellular space like the binding proteins follistatin and FLRG, and at the cell membrane antagonistic co-receptors like Cripto or BAMBI. Additionally, in the intracellular space inhibitory Smads can modulate and control activin activity. Accumulating data suggest that deregulation of activin signals contributes to pathologic conditions such as chronic inflammation, fibrosis and development of cancer. The current article reviews the alterations in components of the activin signaling pathway that have been observed in HCC and discusses their potential significance for liver tumorigenesis.
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