PDGFRA 突变胚胎中的心脏畸形与第二心脏场中 WT1 和 NKX2.5 的表达增加有关。
Cardiac malformations in Pdgfralpha mutant embryos are associated with increased expression of WT1 and Nkx2.5 in the second heart field.
机构信息
Department of Anatomy and Embryology, Leiden University Medical Center, 2300 RC Leiden, The Netherlands.
出版信息
Dev Dyn. 2010 Aug;239(8):2307-17. doi: 10.1002/dvdy.22363.
Abstract
Platelet-derived growth factor receptor alpha (Pdgfralpha) identifies cardiac progenitor cells in the posterior part of the second heart field. We aim to elucidate the role of Pdgfralpha in this region. Hearts of Pdgfralpha-deficient mouse embryos (E9.5-E14.5) showed cardiac malformations consisting of atrial and sinus venosus myocardium hypoplasia, including venous valves and sinoatrial node. In vivo staining for Nkx2.5 showed increased myocardial expression in Pdgfralpha mutants, confirmed by Western blot analysis. Due to hypoplasia of the primary atrial septum, mesenchymal cap, and dorsal mesenchymal protrusion, the atrioventricular septal complex failed to fuse. Impaired epicardial development and severe blebbing coincided with diminished migration of epicardium-derived cells and myocardial thinning, which could be linked to increased WT1 and altered alpha4-integrin expression. Our data provide novel insight for a possible role for Pdgfralpha in transduction pathways that lead to repression of Nkx2.5 and WT1 during development of posterior heart field-derived cardiac structures.
摘要
血小板衍生生长因子受体α(Pdgfralpha)可识别第二心区后部的心脏祖细胞。我们旨在阐明 Pdgfralpha 在该区域的作用。Pdgfralpha 缺陷型小鼠胚胎(E9.5-E14.5)的心脏表现出心脏畸形,包括心房和窦房结心肌发育不良,包括静脉瓣和窦房结。体内 Nkx2.5 染色显示 Pdgfralpha 突变体的心肌表达增加,Western blot 分析证实了这一点。由于原发房间隔、间质帽和背侧间质突起的发育不良,房室间隔复合体未能融合。心外膜发育受损和严重起泡与心外膜衍生细胞的迁移减少以及心肌变薄同时发生,这可能与 WT1 增加和α4-整合素表达改变有关。我们的数据为 Pdgfralpha 在信号通路中的可能作用提供了新的见解,这些信号通路导致 Nkx2.5 和 WT1 在第二心区源性心脏结构发育过程中的表达受到抑制。
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