An endothelial SOX18-mevalonate pathway axis enables repurposing of statins for infantile hemangioma

Author:

Holm AnnegretORCID,Graus Matthew S.ORCID,Wylie-Sears JillORCID,Borgelt Luke,Heng Tan Jerry Wei,Nasim SanaORCID,Chung Long,Jain Ashish,Sun Mingwei,Sun Liang,Brouillard PascalORCID,Lekwuttikarn Ramrada,Kozakewich Harry,Qi Jacob YanfeiORCID,Teng Joyce C.,Mulliken John B.,Vikkula MiikkaORCID,Francois MathiasORCID,Bischoff JoyceORCID

Abstract

ABSTRACTInfantile hemangioma (IH) is the most common tumor in children and a paradigm for pathological vasculogenesis, angiogenesis and regression. Propranolol is the mainstay of treatment for IH. It inhibits hemangioma vessel formation via a β-adrenergic receptor independent off-target effect of its R(+) enantiomer on the endothelial specific transcription factor sex-determining region Y (SRY) box transcription factor 18 (SOX18). Transcriptomic profiling of patient-derived hemangioma stem cells uncovered the mevalonate pathway (MVP) as a target of R(+) propranolol. Loss of SOX18 function confirmed R(+) propranolol mode of action on the MVP. Functional validation in preclinical IH models revealed that statins - targeting the MVP - are potent inhibitors of hemangioma vessel formation. We propose a novel SOX18-MVP-axis as a central regulator of IH pathogenesis and suggest statin repurposing to treat IH. Our findings reveal novel pleiotropic effects of beta-blockers and statins acting on the SOX18-MVP axis to disable an endothelial specific program in IH, which may impact other scenarios involving pathological vasculogenesis and angiogenesis.Graphical abstract

Publisher

Cold Spring Harbor Laboratory

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