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心脏内皮细胞的异质性决定了瓣膜发育,这一点通过心内膜垫组织抗原JB3的不同表达得以证明。

Cardiac endothelial heterogeneity defines valvular development as demonstrated by the diverse expression of JB3, an antigen of the endocardial cushion tissue.

作者信息

Wunsch A M, Little C D, Markwald R R

机构信息

Department of Cellular Biology and Anatomy, Medical College of Wisconsin, Milwaukee 53226.

出版信息

Dev Biol. 1994 Oct;165(2):585-601. doi: 10.1006/dbio.1994.1278.

Abstract

The endothelium of the embryonic vertebrate heart evokes a regional specificity that remains an unexplained phenomenon in cardiac morphogenesis. A restricted population of endothelial cells lining the atrioventricular (AV) canal and proximal outflow tract (OT) transforms into mesenchyme, the reputed progenitor of the valves and membranous septa. The remainder of the cells lining these and other regions of the heart, in particular the ventricle, stay epithelial. At the present time there is no information regarding the determinants for endothelial cell diversity. To investigate the molecular basis for functionally distinct endothelial cell populations, we undertook a search for cell surface proteins within the endocardial cushions of Day 4 chicken embryos that might be sensitive to subtle differences in endothelial cell composition. We theorized that monoclonal antibodies raised against proteins expressed during early valve morphogenesis could provide markers for endothelial subpopulations, thereby assisting our efforts in defining, and determining the origin of, endothelial heterogeneity. In the present study, an in vitro collagen gel culture assay was employed to identify an antibody, JB3, that distinguishes between AV/OT endothelium and ventricular endothelium. Based on this assay, JB3-positive material was associated only with AV/OT endothelia or the mesenchyme derived from these epithelia. Also, a network of JB3-positive fibrillar material was observed within the collagen gel surrounding the explanted cells. The JB3 antigen showed a conspicuous distribution in pregastrulation-stage chicken embryos with immunolabeling observed in the initial primitive streak at 5 hr incubation (stage 2). Subsequent detection in the definitive primitive streak, Hensen's mode, and notochord indicate a consistent relationship to midline structures. JB3 antigen also localized to the regions of presumptive precardiac mesoderm and, at later stages, neural crest, somites, and ventral mesocardium. These data suggest that the JB3 antigen may play a role in establishing cardiac endothelial diversity by defining a subpopulation of cells destined to participate in valve formation. Moreover, JB3 may also influence formation of the primary axis and mesoderm structures that form at the midline. Immunochemical analyses showed that JB3 recognizes a polypeptide that migrates near the molecular weight position of fibrillin (350-390 kDa), the extracellular matrix protein linked to the Marfan syndrome. Based on the molecular mass and similar immunostaining patterns in early embryos, we propose that the JB3 antigen is a fibrillin isotype or a fibrillin-associated protein.

摘要

胚胎脊椎动物心脏的内皮细胞引发了一种区域特异性,这在心脏形态发生过程中仍是一个无法解释的现象。位于房室(AV)管和近端流出道(OT)的有限数量的内皮细胞会转变为间充质,间充质是瓣膜和膜性间隔的公认祖细胞。心脏这些区域和其他区域(特别是心室)的其余细胞则保持上皮状态。目前,尚无关于内皮细胞多样性决定因素的信息。为了研究功能不同的内皮细胞群体的分子基础,我们在第4天鸡胚的心内膜垫中寻找可能对内皮细胞组成的细微差异敏感的细胞表面蛋白。我们推测,针对早期瓣膜形态发生过程中表达的蛋白质产生的单克隆抗体可以为内皮亚群提供标记,从而有助于我们定义和确定内皮异质性的来源。在本研究中,采用体外胶原凝胶培养试验来鉴定一种抗体JB3,它能区分AV/OT内皮细胞和心室内皮细胞。基于该试验,JB3阳性物质仅与AV/OT内皮细胞或源自这些上皮细胞的间充质相关。此外,在植入细胞周围的胶原凝胶中观察到了JB3阳性纤维状物质网络。JB3抗原在原肠胚形成前阶段的鸡胚中显示出明显的分布,在孵化5小时(第2阶段)的初始原条中观察到免疫标记。随后在确定的原条、亨森结和脊索中的检测表明与中线结构存在一致的关系。JB3抗原也定位于推定的心前中胚层区域,在后期定位于神经嵴、体节和腹侧心内膜。这些数据表明,JB3抗原可能通过定义注定参与瓣膜形成的细胞亚群,在建立心脏内皮细胞多样性中发挥作用。此外,JB3也可能影响原轴和在中线形成的中胚层结构的形成。免疫化学分析表明,JB3识别一种迁移到原纤维蛋白(350 - 390 kDa)分子量位置附近的多肽,原纤维蛋白是与马凡综合征相关的细胞外基质蛋白。基于早期胚胎中的分子量和相似的免疫染色模式,我们提出JB3抗原是一种原纤维蛋白同种型或原纤维蛋白相关蛋白。

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