Liver sinusoidal endothelial cells contribute to portal hypertension through collagen type IV-driven sinusoidal remodeling

Portal hypertension (PHTN) is a severe complication of liver cirrhosis and is associated with intrahepatic sinusoidal remodeling induced by sinusoidal resistance and angiogenesis. Collagen type IV (COL4), a major component of basement membrane, forms in liver sinusoids upon chronic liver injury. How...

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Bibliographic Details
Published in:JCI insight 2024-05, Vol.9 (11)
Main Authors: Gan, Can, Yaqoob, Usman, Lu, Jianwen, Xie, Man, Anwar, Abid, Jalan-Sakrikar, Nidhi, Jerez, Sofia, Sehrawat, Tejasav S, Navarro-Corcuera, Amaia, Kostallari, Enis, Habash, Nawras W, Cao, Sheng, Shah, Vijay H
Format: Article
Language:English
Subjects:
Animals
Collagen Type IV - genetics
Collagen Type IV - metabolism
Endothelial Cells - metabolism
Endothelial Cells - pathology
Epigenesis, Genetic
Humans
Hypertension, Portal - genetics
Hypertension, Portal - metabolism
Hypertension, Portal - pathology
Liver - blood supply
Liver - metabolism
Liver - pathology
Liver Cirrhosis - genetics
Liver Cirrhosis - metabolism
Liver Cirrhosis - pathology
Male
Mice
Mice, Inbred C57BL
NF-kappa B - metabolism
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Summary:Portal hypertension (PHTN) is a severe complication of liver cirrhosis and is associated with intrahepatic sinusoidal remodeling induced by sinusoidal resistance and angiogenesis. Collagen type IV (COL4), a major component of basement membrane, forms in liver sinusoids upon chronic liver injury. However, the role, cellular source, and expression regulation of COL4 in liver diseases are unknown. Here, we examined how COL4 is produced and how it regulates sinusoidal remodeling in fibrosis and PHTN. Human cirrhotic liver sample RNA sequencing showed increased COL4 expression, which was further verified via immunofluorescence staining. Single-cell RNA sequencing identified liver sinusoidal endothelial cells (LSECs) as the predominant source of COL4 upregulation in mouse fibrotic liver. In addition, COL4 was upregulated in a TNF-α/NF-κB-dependent manner through an epigenetic mechanism in LSECs in vitro. Indeed, by utilizing a CRISPRi-dCas9-KRAB epigenome-editing approach, epigenetic repression of the enhancer-promoter interaction showed silencing of COL4 gene expression. LSEC-specific COL4 gene mutation or repression in vivo abrogated sinusoidal resistance and angiogenesis, which thereby alleviated sinusoidal remodeling and PHTN. Our findings reveal that LSECs promote sinusoidal remodeling and PHTN during liver fibrosis through COL4 deposition.
ISSN:2379-3708
2379-3708
DOI:10.1172/jci.insight.174775