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. 2024 Nov;27(4):765-777.
doi: 10.1007/s10456-024-09936-6. Epub 2024 Jul 2.

ACVR1/ALK2-p21 signaling axis modulates proliferation of the venous endothelium in the retinal vasculature

Boryeong Pak #  1 Minjung Kim #  1 Orjin Han #  1 Heon-Woo Lee #  2   3 Alexandre Dubrac  2   4 Woosoung Choi  1 Jee Myung Yang  5 Kevin Boyé  2 Heewon Cho  1 Kathryn M Citrin  6 Injune Kim  5 Anne Eichmann  2 Victoria L Bautch  6 Suk-Won Jin  7   8
Affiliations

ACVR1/ALK2-p21 signaling axis modulates proliferation of the venous endothelium in the retinal vasculature

Boryeong Pak et al. Angiogenesis. 2024 Nov.

Abstract

The proliferation of the endothelium is a highly coordinated process to ensure the emergence, expansion, and homeostasis of the vasculature. While Bone Morphogenetic Protein (BMP) signaling fine-tunes the behaviors of endothelium in health and disease, how BMP signaling influences the proliferation of endothelium and therefore, modulates angiogenesis remains largely unknown. Here, we evaluated the role of Activin A Type I Receptor (ACVR1/ALK2), a key BMP receptor in the endothelium, in modulating the proliferation of endothelial cells. We show that ACVR1/ALK2 is a key modulator for the proliferation of endothelium in the retinal vessels. Loss of endothelial ALK2 leads to a significant reduction in endothelial proliferation and results in fewer branches/endothelial cells in the retinal vessels. Interestingly, venous endothelium appears to be more susceptible to ALK2 deletion. Mechanistically, ACVR1/ALK2 inhibits the expression of CDKN1A/p21, a critical negative regulator of cell cycle progression, in a SMAD1/5-dependent manner, thereby enabling the venous endothelium to undergo active proliferation by suppressing CDKN1A/p21. Taken together, our findings show that BMP signaling mediated by ACVR1/ALK2 provides a critical yet previously underappreciated input to modulate the proliferation of venous endothelium, thereby fine-tuning the context of angiogenesis in health and disease.

Keywords: ALK2/ACVR1; BMP signaling; Cell cycle; Endothelium; p21/CDKN1A.

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Conflict of interest statement

Declarations Competing interests None.

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