Type-H endothelial cell protein Clec14a orchestrates osteoblast activity during trabecular bone formation and patterning

H型内皮细胞蛋白Clec14a在骨小梁形成和模式形成过程中调控成骨细胞活性

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作者:Georgiana Neag ,Jonathan Lewis ,Jason D Turner ,Julia E Manning ,Isaac Dean ,Melissa Finlay ,Gowsihan Poologasundarampillai ,Jonathan Woods ,Muhammad Arham Sahu ,Kabir A Khan ,Jenefa Begum ,Helen M McGettrick ,Ilaria Bellantuono ,Victoria Heath ,Simon W Jones ,Christopher D Buckley ,Roy Bicknell ,Amy J Naylor

Abstract

Type-H capillary endothelial cells control bone formation during embryogenesis and postnatal growth but few signalling mechanisms underpinning this influence have been characterised. Here, we identify a highly expressed type-H endothelial cell protein, Clec14a, and explore its role in coordinating osteoblast activity. Expression of Clec14a and its ligand, Mmrn2 are high in murine type-H endothelial cells but absent from osteoblasts. Clec14a-/- mice have premature condensation of the type-H vasculature and expanded distribution of osteoblasts and bone matrix, increased long-bone length and bone density indicative of accelerated skeletal development, and enhanced osteoblast maturation. Antibody-mediated blockade of the Clec14a-Mmrn2 interaction recapitulates the Clec14a-/- phenotype. Endothelial cell expression of Clec14a regulates osteoblast maturation and mineralisation activity during postnatal bone development in mice. This finding underscores the importance of type-H capillary control of osteoblast activity in bone formation and identifies a novel mechanism that mediates this vital cellular crosstalk.

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