Heterogeneity of hepatocyte dynamics restores liver architecture after chemical, physical or viral damage

肝细胞动力学的异质性可在化学、物理或病毒损伤后恢复肝脏结构。

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作者:Inmaculada Ruz-Maldonado ,John T Gonzalez ,Hanming Zhang ,Jonathan Sun ,Alicia Bort ,Inamul Kabir ,Richard G Kibbey ,Yajaira Suárez ,Daniel M Greif ,Carlos Fernández-Hernando

Abstract

Midlobular hepatocytes are proposed to be the most plastic hepatic cell, providing a reservoir for hepatocyte proliferation during homeostasis and regeneration. However, other mechanisms beyond hyperplasia have been little explored and the contribution of other hepatocyte subpopulations to regeneration has been controversial. Thus, re-examining hepatocyte dynamics during regeneration is critical for cell therapy and treatment of liver diseases. Using a mouse model of hepatocyte- and non-hepatocyte- multicolor lineage tracing, we demonstrate that midlobular hepatocytes also undergo hypertrophy in response to chemical, physical, and viral insults. Our study shows that this subpopulation also combats liver impairment after infection with coronavirus. Furthermore, we demonstrate that pericentral hepatocytes also expand in number and size during the repair process and Galectin-9-CD44 pathway may be critical for driving these processes. Notably, we also identified that transdifferentiation and cell fusion during regeneration after severe injury contribute to recover hepatic function.

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