Sulfide oxidation promotes hypoxic angiogenesis and neovascularization.
Roshan KumarVictor VitvitskyApichaya SethaudomRashi SinghalSumeet SolankiSydney AlibeckoffHarrison L HirakiHannah N BellAnthony AndrenBrendon M BakerCostas A LyssiotisYatrik M ShahRuma BanerjeePublished in: Nature chemical biology (2024)
Angiogenic programming in the vascular endothelium is a tightly regulated process for maintaining tissue homeostasis and is activated in tissue injury and the tumor microenvironment. The metabolic basis of how gas signaling molecules regulate angiogenesis is elusive. Here, we report that hypoxic upregulation of ·NO in endothelial cells reprograms the transsulfuration pathway to increase biogenesis of hydrogen sulfide (H 2 S), a proangiogenic metabolite. However, decreased H 2 S oxidation due to sulfide quinone oxidoreductase (SQOR) deficiency synergizes with hypoxia, inducing a reductive shift and limiting endothelial proliferation that is attenuated by dissipation of the mitochondrial NADH pool. Tumor xenografts in whole-body (WB Cre Sqor fl/fl ) and endothelial-specific (VE-cadherin Cre-ERT2 Sqor fl/fl ) Sqor-knockout mice exhibit lower mass and angiogenesis than control mice. WB Cre Sqor fl/fl mice also exhibit decreased muscle angiogenesis following femoral artery ligation compared to control mice. Collectively, our data reveal the molecular intersections between H 2 S, O 2 and ·NO metabolism and identify SQOR inhibition as a metabolic vulnerability for endothelial cell proliferation and neovascularization.