CRIM1 is necessary for coronary vascular endothelial cell development and homeostasis

被引:0
作者
Swati Iyer
Yash Chhabra
Tracey J. Harvey
Richard Wang
Han Sheng Chiu
A. G. Smith
Walter G. Thomas
David J. Pennisi
Michael Piper
机构
[1] The University of Queensland,School of Biomedical Sciences
[2] The University of Queensland,Queensland Brain Institute
来源
Journal of Molecular Histology | 2017年 / 48卷
关键词
Heart; Endothelial cells;
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中图分类号
学科分类号
摘要
Endothelial cells form a critical component of the coronary vasculature, yet the factors regulating their development remain poorly defined. Here we reveal a novel role for the transmembrane protein CRIM1 in mediating cardiac endothelial cell development. In the absence of Crim1 in vivo, the coronary vasculature is malformed, the number of endothelial cells reduced, and the canonical BMP pathway dysregulated. Moreover, we reveal that CRIM1 can bind IGFs, and regulate IGF signalling within endothelial cells. Finally, loss of CRIM1 from human cardiac endothelial cells results in misregulation of endothelial genes, predicted by pathway analysis to be involved in an increased inflammatory response and cytolysis, reminiscent of endothelial cell dysfunction in cardiovascular disease pathogenesis. Collectively, these findings implicate CRIM1 in endothelial cell development and homeostasis in the coronary vasculature.
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页码:53 / 61
页数:8
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