ALK1 controls hepatic vessel formation, angiodiversity, and angiocrine functions in hereditary hemorrhagic telangiectasia of the liver

Christian David Schmid; Victor Olsavszky; Manuel Reinhart; Vanessa Weyer; Felix A. Trogisch; Carsten Sticht; Manuel Winkler; Sina W. Kürschner; Johannes Hoffmann; Roxana Ola; Theresa Staniczek; Joerg Heineke; Beate K. Straub; Jens Mittler; Kai Schledzewski; Peter ten Dijke; Karsten Richter; Steven Dooley; Cyrill Géraud; Sergij Goerdt; Philipp‐Sebastian Koch

doi:10.1002/hep.32641

ALK1 controls hepatic vessel formation, angiodiversity, and angiocrine functions in hereditary hemorrhagic telangiectasia of the liver

Christian David Schmid(Heidelberg University), Victor Olsavszky(Heidelberg University), Manuel Reinhart(Heidelberg University), Vanessa Weyer(Heidelberg University), Felix A. Trogisch(Heidelberg University), Carsten Sticht(Heidelberg University), Manuel Winkler(Heidelberg University), Sina W. Kürschner(Heidelberg University), Johannes Hoffmann(Heidelberg University), Roxana Ola(Heidelberg University), Theresa Staniczek(Heidelberg University), Joerg Heineke(Heidelberg University), Beate K. Straub(Johannes Gutenberg University Mainz), Jens Mittler(Johannes Gutenberg University Mainz), Kai Schledzewski(Heidelberg University), Peter ten Dijke(Leiden University Medical Center), Karsten Richter(German Cancer Research Center), Steven Dooley(Heidelberg University), Cyrill Géraud(Heidelberg University), Sergij Goerdt(Heidelberg University), Philipp‐Sebastian Koch(Heidelberg University)

Hepatology

July 1, 2022

10.1002/hep.32641

Cited by 35Open Access

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Abstract

BACKGROUND AND AIMS: In hereditary hemorrhagic telangiectasia (HHT), severe liver vascular malformations are associated with mutations in the Activin A Receptor-Like Type 1 ( ACVRL1 ) gene encoding ALK1, the receptor for bone morphogenetic protein (BMP) 9/BMP10, which regulates blood vessel development. Here, we established an HHT mouse model with exclusive liver involvement and adequate life expectancy to investigate ALK1 signaling in liver vessel formation and metabolic function. APPROACH AND RESULTS: Liver sinusoidal endothelial cell (LSEC)-selective Cre deleter line, Stab2-iCreF3 , was crossed with Acvrl1 -floxed mice to generate LSEC-specific Acvrl1 -deficient mice ( Alk1HEC-KO ). Alk1HEC-KO mice revealed hepatic vascular malformations and increased posthepatic flow, causing right ventricular volume overload. Transcriptomic analyses demonstrated induction of proangiogenic/tip cell gene sets and arterialization of hepatic vessels at the expense of LSEC and central venous identities. Loss of LSEC angiokines Wnt2 , Wnt9b , and R-spondin-3 ( Rspo3 ) led to disruption of metabolic liver zonation in Alk1HEC-KO mice and in liver specimens of patients with HHT. Furthermore, prion-like protein doppel ( Prnd ) and placental growth factor ( Pgf ) were upregulated in Alk1HEC-KO hepatic endothelial cells, representing candidates driving the organ-specific pathogenesis of HHT. In LSEC in vitro , stimulation or inhibition of ALK1 signaling counter-regulated Inhibitors of DNA binding (ID)1-3, known Alk1 transcriptional targets. Stimulation of ALK1 signaling and inhibition of ID1-3 function confirmed regulation of Wnt2 and Rspo3 by the BMP9/ALK1/ID axis. CONCLUSIONS: Hepatic endothelial ALK1 signaling protects from development of vascular malformations preserving organ-specific endothelial differentiation and angiocrine signaling. The long-term surviving Alk1HEC-KO HHT model offers opportunities to develop targeted therapies for this severe disease.

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