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ErbB2 促进人左心室心外膜高增殖细胞(eHiPC)的内皮表型。

ErbB2 promotes endothelial phenotype of human left ventricular epicardial highly proliferative cells (eHiPC).

机构信息

Maine Medical Center Research Institute, Scarborough, ME, United States.

Maine Medical Center Research Institute, Scarborough, ME, United States; Maine Medical Center, Portland, ME, United States.

出版信息

J Mol Cell Cardiol. 2018 Feb;115:39-50. doi: 10.1016/j.yjmcc.2017.12.013. Epub 2017 Dec 29.

Abstract

The adult human heart contains a subpopulation of highly proliferative cells. The role of ErbB receptors in these cells has not been studied. From human left ventricular (LV) epicardial biopsies, we isolated highly proliferative cells (eHiPC) to characterize the cell surface expression and function of ErbB receptors in the regulation of cell proliferation and phenotype. We found that human LV eHiPC express all four ErbB receptor subtypes. However, the expression of ErbB receptors varied widely among eHiPC isolated from different subjects. eHiPC with higher cell surface expression of ErbB2 reproduced the phenotype of endothelial cells and were characterized by endothelial cell-like functional properties. We also found that EGF/ErbB1 induces VEGFR2 expression, while ligands for both ErbB1 and ErbB3/4 induce expression of Tie2. The number of CD31CD45 endothelial cells is higher in LV biopsies from subjects with high ErbB2 (ErbB2) eHiPC compared to low ErbB2 (ErbB2) eHiPC. These findings have important implications for potential strategies to increase the efficacy of cell-based revascularization of the injured heart, through promotion of an endothelial phenotype in cardiac highly proliferative cells.

摘要

成人心脏包含一群具有高度增殖能力的细胞。目前尚未研究 ErbB 受体在这些细胞中的作用。我们从人类左心室心外膜活检组织中分离出具有高度增殖能力的细胞(eHiPC),以研究 ErbB 受体在调节细胞增殖和表型中的作用。我们发现,人左心室 eHiPC 表达所有四种 ErbB 受体亚型。然而,不同个体来源的 eHiPC 中 ErbB 受体的表达差异很大。eHiPC 中 ErbB2 的细胞表面表达水平较高,复制了内皮细胞的表型,并具有内皮细胞样的功能特性。我们还发现,EGF/ErbB1 诱导 VEGFR2 的表达,而 ErbB1 和 ErbB3/4 的配体均可诱导 Tie2 的表达。与低 ErbB2(ErbB2)eHiPC 相比,高 ErbB2(ErbB2)eHiPC 的 LV 活检组织中 CD31CD45 内皮细胞数量更高。这些发现对于通过促进心脏高增殖细胞的内皮表型来提高基于细胞的损伤心脏再血管化效果的潜在策略具有重要意义。

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