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肝脏再生和生长稳态的原则。

Principles of liver regeneration and growth homeostasis.

机构信息

Department of Pathology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA.

出版信息

Compr Physiol. 2013 Jan;3(1):485-513. doi: 10.1002/cphy.c120014.

Abstract

Liver regeneration is perhaps the most studied example of compensatory growth aimed to replace loss of tissue in an organ. Hepatocytes, the main functional cells of the liver, manage to proliferate to restore mass and to simultaneously deliver all functions hepatic functions necessary to maintain body homeostasis. They are the first cells to respond to regenerative stimuli triggered by mitogenic growth factor receptors MET (the hepatocyte growth factor receptor] and epidermal growth factor receptor and complemented by auxiliary mitogenic signals induced by other cytokines. Termination of liver regeneration is a complex process affected by integrin mediated signaling and it restores the organ to its original mass as determined by the needs of the body (hepatostat function). When hepatocytes cannot proliferate, progenitor cells derived from the biliary epithelium transdifferentiate to restore the hepatocyte compartment. In a reverse situation, hepatocytes can also transdifferentiate to restore the biliary compartment. Several hormones and xenobiotics alter the hepatostat directly and induce an increase in liver to body weight ratio (augmentative hepatomegaly). The complex challenges of the liver toward body homeostasis are thus always preserved by complex but unfailing responses involving orchestrated signaling and affecting growth and differentiation of all hepatic cell types.

摘要

肝脏再生可能是研究最多的代偿性生长的例子,旨在替代组织在器官中的损失。肝细胞是肝脏的主要功能细胞,它们设法增殖以恢复质量,并同时提供维持身体内稳态所需的所有肝脏功能。它们是对由有丝分裂生长因子受体 MET(肝细胞生长因子受体)和表皮生长因子受体触发的再生刺激作出反应的第一类细胞,并辅以其他细胞因子诱导的辅助有丝分裂信号。肝脏再生的终止是一个复杂的过程,受整合素介导的信号转导影响,并根据身体的需要将器官恢复到原始质量(肝稳态功能)。当肝细胞不能增殖时,来源于胆管上皮的祖细胞转分化以恢复肝细胞区室。在相反的情况下,肝细胞也可以转分化以恢复胆管区室。几种激素和外源性物质直接改变肝稳态,并导致肝脏与体重比增加(代偿性肝肿大)。因此,肝脏对身体内稳态的复杂挑战始终通过涉及协调信号转导的复杂但可靠的反应来保存,影响所有肝实质细胞类型的生长和分化。

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