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Prometheus revisited: liver homeostasis and repair

机译:普罗米修斯再访:肝脏稳态与修复

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摘要

The liver is a bioreactor responsible for metabolism of nutrients and xenobiotics, as well as a factory and recycling station for a large number of systemic proteins. Its unmatched regenerative capacity was already described in the myth of Prometheus 2500 years ago and extensively studied over the past decades. However, the exact mechanisms enabling maintenance of liver mass during homeostasis and repair remained unclear. Diploid glutamine synthetase (GS)+ pericentral hepatocytes expressing the WNT/β-Catenin target gene showed superior proliferative capacity over mostly polyploid hepatocytes in other zones. These GS+/AXIN2+ pericentral hepatocytes were considered liver stem cells as they self-renewed and replaced all hepatocytes along the liver lobule during homeostatic renewal [ ]. In contrast, lineage tracing using , another WNT/β-Catenin target gene and pericentral hepatocyte marker, did not support increased proliferative capacity and expansion of pericentral hepatocytes into other zones [ , ]. Likewise, mTERT lineage tracing suggested no zonal dominance of pericentral hepatocytes during liver homeostasis but proposed self-renewing mTERT hepatocytes with increased proliferative capacity as liver stem cells [ ]. Moreover, SOX9+ periportal hepatocytes were described as hybrid hepatocytes with liver stem cell properties as they displayed increased regenerative potential in response to injury [ ]. The controversy around the elusive liver stem cell arises from the diverse hepatocyte populations that have been proposed to harbor increased regenerative capacity and the conflicting results originating from different lineage tracing experiments under different housing conditions [ – ]
机译:肝脏是负责营养物质和异生物素代谢的生物反应器,也是大量系统蛋白的工厂和回收站。其无与伦比的再生能力已在2500年前的普罗米修斯神话中得到描述,并在过去的几十年中得到了广泛的研究。但是,尚不清楚在体内动态平衡和修复过程中能否维持肝脏肿块的确切机制。表达WNT /β-Catenin靶标基因的二倍体谷氨酰胺合成酶(GS)+中央肝细胞显示出比其他区域中大多数多倍体肝细胞优越的增殖能力。这些GS + / AXIN2 +外周肝细胞被认为是肝脏干细胞,因为它们自我更新并在稳态更新过程中替换了沿肝小叶的所有肝细胞。相比之下,使用另一个WNT /β-Catenin靶基因和中枢肝细胞标志物进行谱系追踪并不支持增加的增殖能力和中枢肝细胞向其他区域的扩展[,]。同样,mTERT谱系示踪表明肝稳态期间无中央区肝细胞的区域优势,但提出了自我更新的mTERT肝细胞作为肝干细胞具有增强的增殖能力[]。此外,SOX9 +肝门周围肝细胞被描述为具有肝干细胞特性的杂合肝细胞,因为它们显示出对损伤反应的再生潜力增加[]。难以捉摸的肝干细胞引起的争议是由各种各样的肝细胞种群引起的,这些种群被认为具有增加的再生能力,并且在不同的居住条件下源自不同的血统追踪实验产生了矛盾的结果[–]

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