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Wnt信号通路通过腱生蛋白C/血小板衍生生长因子受体途径调节小鼠肺中平滑肌前体细胞的发育。

Wnt signaling regulates smooth muscle precursor development in the mouse lung via a tenascin C/PDGFR pathway.

作者信息

Cohen Ethan David, Ihida-Stansbury Kaori, Lu Min Min, Panettieri Reynold A, Jones Peter Lloyd, Morrisey Edward E

机构信息

Department of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104, USA.

出版信息

J Clin Invest. 2009 Sep;119(9):2538-49. doi: 10.1172/JCI38079. Epub 2009 Aug 17.

Abstract

Paracrine signaling from lung epithelium to the surrounding mesenchyme is important for lung SMC development and function and is a contributing factor in an array of pulmonary diseases such as bronchopulmonary dysplasia, pulmonary hypertension, and asthma. Wnt7b, which is exclusively expressed in the lung epithelium, is important for lung vascular smooth muscle integrity, but the underlying mechanism by which Wnt signaling regulates lung SMC development is unclear. In this report, we have demonstrated that Wnt7b regulates a program of mesenchymal differentiation in the mouse lung that is essential for SMC development. Genetic loss-of-function studies showed that Wnt7b and beta-catenin were required for expression of Pdgfralpha and Pdgfrbeta and proliferation in pulmonary SMC precursors. In contrast, gain-of-function studies showed that activation of Wnt signaling increased the expression of both Pdgfralpha and Pdgfrbeta as well as the proliferation of SMC precursors. We further showed that the effect on Pdgfr expression was, in part, mediated by direct transcriptional regulation of the ECM protein tenascin C (Tnc), which was necessary and sufficient for Pdgfralpha/beta expression in lung explants. Moreover, this pathway was highly upregulated in a mouse model of asthma and in lung tissue from patients with pulmonary hypertension. Together, these data define a Wnt/Tnc/Pdgfr signaling axis that is critical for smooth muscle development and disease progression in the lung.

摘要

从肺上皮细胞到周围间充质的旁分泌信号传导对于肺平滑肌细胞的发育和功能很重要,并且是一系列肺部疾病(如支气管肺发育不良、肺动脉高压和哮喘)的一个促成因素。仅在肺上皮细胞中表达的Wnt7b对于肺血管平滑肌的完整性很重要,但Wnt信号传导调节肺平滑肌细胞发育的潜在机制尚不清楚。在本报告中,我们证明Wnt7b调节小鼠肺中间充质分化程序,这对平滑肌细胞发育至关重要。基因功能丧失研究表明,Wnt7b和β-连环蛋白是肺平滑肌细胞前体中血小板衍生生长因子受体α(Pdgfralpha)和血小板衍生生长因子受体β(Pdgfrbeta)表达及增殖所必需的。相反,功能获得研究表明,Wnt信号激活增加了Pdgfralpha和Pdgfrbeta的表达以及平滑肌细胞前体的增殖。我们进一步表明,对血小板衍生生长因子受体(Pdgfr)表达的影响部分是由细胞外基质蛋白腱生蛋白C(Tnc)的直接转录调控介导的,Tnc对于肺外植体中Pdgfralpha/beta的表达是必需且充分的。此外,该通路在哮喘小鼠模型和肺动脉高压患者的肺组织中高度上调。总之,这些数据定义了一个对肺平滑肌发育和疾病进展至关重要的Wnt/Tnc/Pdgfr信号轴。

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