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β-连环蛋白信号通路在生理性肝脏生长过程中的作用与调控

Role and regulation of β-catenin signaling during physiological liver growth.

作者信息

Monga Satdarshan Paul Singh

机构信息

Department of Pathology and Medicine, University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.

出版信息

Gene Expr. 2014;16(2):51-62. doi: 10.3727/105221614X13919976902138.

Abstract

Wnt/β-catenin signaling plays key roles not only during development but also in adult tissue homeostasis. This is also evident in liver biology where many temporal roles of β-catenin have been identified during hepatic development, where, in hepatic progenitors or hepatoblasts, it is a key determinant of proliferation and eventually differentiation to mature hepatocytes, while also playing an important role in bile duct homeostasis. β-Catenin signaling cascade is mostly quiescent in hepatocytes in an adult liver except in the centrizonal region of a hepatic lobule. This small rim of hepatocytes around the central vein show constitutive β-catenin activation that in turn regulates expression of genes whose products play an important role in ammonia and xenobiotic metabolism. Intriguingly, β-catenin can also undergo activation in hepatocytes after acute liver loss secondary to surgical or toxicant insult. Such activation of this progrowth protein is observed as nuclear translocation of β-catenin and formation of its complex with the T-cell factor (TCF) family of transcription factors. Expression of cyclin-D1, a key inducer of transition from the G1 to S phase of cell cycle, is regulated by β-catenin-TCF complex. Thus, β-catenin activation is absolutely critical in the normal regeneration process of the liver as shown by studies in several models across various species. In the current review, the temporal role and regulation of β-catenin in liver development, metabolic zonation in a basal adult liver, and during the liver regeneration process will be discussed. In addition, the probability of therapeutically regulating β-catenin activity as a possible future treatment strategy for liver insufficiency will also be discussed.

摘要

Wnt/β-连环蛋白信号通路不仅在发育过程中起关键作用,在成体组织稳态维持中也发挥重要作用。这在肝脏生物学中也很明显,在肝脏发育过程中已确定β-连环蛋白具有许多阶段性作用,在肝祖细胞或肝细胞中,它是增殖以及最终分化为成熟肝细胞的关键决定因素,同时在胆管稳态维持中也发挥重要作用。除了肝小叶的中央区带,β-连环蛋白信号级联在成体肝脏的肝细胞中大多处于静止状态。中央静脉周围这一小圈肝细胞显示出组成型β-连环蛋白激活,进而调节其产物在氨和外源性物质代谢中起重要作用的基因的表达。有趣的是,在手术或毒物损伤继发急性肝损伤后,肝细胞中的β-连环蛋白也会被激活。这种促生长蛋白的激活表现为β-连环蛋白的核转位及其与转录因子T细胞因子(TCF)家族形成复合物。细胞周期蛋白D1是细胞周期从G1期过渡到S期的关键诱导因子,其表达受β-连环蛋白-TCF复合物调控。因此,正如在多个物种的几种模型中所进行的研究所表明的那样,β-连环蛋白激活在肝脏的正常再生过程中绝对至关重要。在本综述中,将讨论β-连环蛋白在肝脏发育、基础成体肝脏的代谢分区以及肝脏再生过程中的阶段性作用和调控。此外,还将讨论作为未来可能的肝衰竭治疗策略对β-连环蛋白活性进行治疗性调节的可能性。

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