| Literature DB >> 35364013 |
Jesus Maria Gómez-Salinero1, Franco Izzo2, Yang Lin3, Sean Houghton3, Tomer Itkin3, Fuqiang Geng3, Yaron Bram4, Robert P Adelson5, Tyler M Lu6, Giorgio Inghirami7, Jenny Zhaoying Xiang8, Raphael Lis6, David Redmond3, Ryan Schreiner3, Sina Y Rabbany9, Dan A Landau2, Robert E Schwartz10, Shahin Rafii11.
Abstract
The liver vascular network is patterned by sinusoidal and hepatocyte co-zonation. How intra-liver vessels acquire their hierarchical specialized functions is unknown. We study heterogeneity of hepatic vascular cells during mouse development through functional and single-cell RNA-sequencing. The acquisition of sinusoidal endothelial cell identity is initiated during early development and completed postnatally, originating from a pool of undifferentiated vascular progenitors at E12. The peri-natal induction of the transcription factor c-Maf is a critical switch for the sinusoidal identity determination. Endothelium-restricted deletion of c-Maf disrupts liver sinusoidal development, aberrantly expands postnatal liver hematopoiesis, promotes excessive postnatal sinusoidal proliferation, and aggravates liver pro-fibrotic sensitivity to chemical insult. Enforced c-Maf overexpression in generic human endothelial cells switches on a liver sinusoidal transcriptional program that maintains hepatocyte function. c-Maf represents an inducible intra-organotypic and niche-responsive molecular determinant of hepatic sinusoidal cell identity and lays the foundation for the strategies for vasculature-driven liver repair.Entities:
Keywords: c-Maf; development; endothelial cell reprogramming; endothelial cell specification; fibrosis; hepatic angiocrine factors; liver sinusoidal endothelial cells; postnatal maturation; single-cell RNAseq; single-cell molecular profiling; vascular heterogeneity
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Year: 2022 PMID: 35364013 PMCID: PMC9290393 DOI: 10.1016/j.stem.2022.03.002
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 25.269