Identification of an autocrine signaling pathway that amplifies induction of endocardial cushion tissue in the avian heart.

Acta anatomica Pub Date : 1998-01-01 DOI:10.1159/000046463
A F Ramsdell, R A Moreno-Rodriguez, M M Wienecke, Y Sugi, D K Turner, C H Mjaatvedt, R R Markwald
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引用次数: 21

Abstract

Endocardial cushion tissue is formed by an epithelial-mesenchymal transformation of endocardial cells, a process which results from an inductive interaction between the myocardium and endocardium within the atrioventricular (AV) and outflow tract (OT) regions of the heart. We report here that a protein previously found to be required for myocardially induced transformation of endocardial cells in vitro, ES/130, is highly expressed within the AV and OT regions not only by myocardial cells, but also by the endocardium and its mesenchymal progeny. Given these findings and others, we have tested the hypothesis that endocardial cushion tissue secretes factors which autoregulate its transformation to mesenchyme. Endocardial cushion tissue was cultured and its conditioned growth medium was harvested and applied to nontransformed endocardial cells maintained in the absence of the inductive myocardium. This treatment resulted in endocardial cell invasion into three-dimensional collagen gels plus increased expression of proteins associated with endocardial cell transformation in vivo. Whereas endocardial cushion tissue was found to express ES/130 protein in vivo and in vitro, minimal detection of ES/130 in its conditioned growth medium was observed in immunoblots. Attempts to inhibit the mesenchyme-promoting activity of the conditioned medium with ES/130 antisense were unsuccessful. However, strong intracellular ES/130 expression was detected in endocardial cells, and this expression correlated with the ability of endocardial cells to transform. For example, the minority of endocardial cultures that failed to transform in response to conditioned medium treatment also failed to undergo increased expression of ES/130. These observations are interpreted to suggest that (i) endocardial cushion tissue secretes factors that promote its transformation to mesenchyme, and (ii) while endocardial cushion tissue appears to signal through secretion of factors other than or in addition to ES/130, intracellular ES/130 expression nevertheless may be a target endocardial cell response required for endocardial cell transformation.

鉴定自分泌信号通路,放大诱导心内膜缓冲组织在鸟类心脏。
心内膜缓冲组织是由心内膜细胞的上皮-间质转化形成的,这一过程是由心脏房室(AV)和流出道(OT)区域内心肌和心内膜之间的诱导相互作用引起的。我们在这里报道了一种先前发现的体外心肌诱导心内膜细胞转化所需的蛋白ES/130,不仅在心肌细胞,而且在心内膜及其间充质子代细胞的AV和OT区域内高度表达。鉴于这些发现和其他发现,我们已经测试了心内膜缓冲组织分泌因子自动调节其向间质转化的假设。培养心内膜缓冲组织,收集其条件生长培养基,并将其应用于在没有诱导心肌的情况下维持的未转化的心内膜细胞。这种处理导致心内膜细胞侵入三维胶原凝胶,并且增加了体内与心内膜细胞转化相关的蛋白质的表达。虽然在体内和体外均发现心内膜缓冲组织表达ES/130蛋白,但在免疫印迹中,在其条件生长培养基中几乎检测不到ES/130蛋白。试图用ES/130反义抑制条件培养基的促间质活性均未成功。然而,在心内膜细胞中检测到强烈的细胞内ES/130表达,这种表达与心内膜细胞的转化能力相关。例如,少数心内膜培养物在条件培养基处理下未能转化,也未能增加ES/130的表达。这些观察结果被解释为:(i)心内膜缓冲组织分泌促进其向间质转化的因子,(ii)虽然心内膜缓冲组织似乎通过除ES/130以外的其他因子的分泌来发出信号,但细胞内ES/130的表达可能是心内膜细胞转化所需的靶心内膜细胞反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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