IGFBP2 expressing midlobular hepatocytes preferentially contribute to liver homeostasis and regeneration

表达IGFBP2的中叶肝细胞优先参与肝脏稳态和再生。

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作者:Yu-Hsuan Lin ,Yonglong Wei ,Qiyu Zeng ,Yunguan Wang ,Chase A Pagani ,Lin Li ,Min Zhu ,Zixi Wang ,Meng-Hsiung Hsieh ,Natasha Corbitt ,Yu Zhang ,Tripti Sharma ,Tao Wang ,Hao Zhu

Abstract

Although midlobular hepatocytes in zone 2 are a recently identified cellular source for liver homeostasis and regeneration, these cells have not been exclusively fate mapped. We generated an Igfbp2-CreER knockin strain that specifically labels midlobular hepatocytes. During homeostasis over 1 year, zone 2 hepatocytes increased in abundance from occupying 21%-41% of the lobular area. After either pericentral injury with carbon tetrachloride or periportal injury with 3,5-diethoxycarbonyl-1,4-dihydrocollidine (DDC), IGFBP2+ cells replenished lost hepatocytes in zones 3 and 1, respectively. IGFBP2+ cells also preferentially contributed to regeneration after 70% partial hepatectomy, as well as liver growth during pregnancy. Because IGFBP2 labeling increased substantially with fasting, we used single nuclear transcriptomics to explore zonation as a function of nutrition, revealing that the zonal division of labor shifts dramatically with fasting. These studies demonstrate the contribution of IGFBP2-labeled zone 2 hepatocytes to liver homeostasis and regeneration. Keywords: lineage tracing; midlobular hepatocytes; regeneration; zonation; zone 2.

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