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人类心脏的心房发育:一项着重于间充质组织作用的免疫组织化学研究。

Atrial development in the human heart: an immunohistochemical study with emphasis on the role of mesenchymal tissues.

作者信息

Wessels A, Anderson R H, Markwald R R, Webb S, Brown N A, Viragh S, Moorman A F, Lamers W H

机构信息

Department of Cell Biology and Anatomy, Medical University of South Carolina, Charleston 29425, USA.

出版信息

Anat Rec. 2000 Jul 1;259(3):288-300. doi: 10.1002/1097-0185(20000701)259:3<288::AID-AR60>3.0.CO;2-D.

Abstract

The development of the atrial chambers in the human heart was investigated immunohistochemically using a set of previously described antibodies. This set included the monoclonal antibody 249-9G9, which enabled us to discriminate the endocardial cushion-derived mesenchymal tissues from those derived from extracardiac splanchnic mesoderm, and a monoclonal antibody recognizing the B isoform of creatine kinase, which allowed us to distinguish the right atrial myocardium from the left. The expression patterns obtained with these antibodies, combined with additional histological information derived from the serial sections, permitted us to describe in detail the morphogenetic events involved in the development of the primary atrial septum (septum primum) and the pulmonary vein in human embryos from Carnegie stage 14 onward. The level of expression of creatine kinase B (CK-B) was found to be consistently higher in the left atrial myocardium than in the right, with a sharp boundary between high and low expression located between the primary septum and the left venous valve indicating that the primary septum is part of the left atrial gene-expression domain. This expression pattern of CK-B is reminiscent of that of the homeobox gene Pitx2, which has recently been shown to be important for atrial septation in the mouse. This study also demonstrates a poorly appreciated role of the dorsal mesocardium in cardiac development. From the earliest stage investigated onward, the mesenchyme of the dorsal mesocardium protrudes into the dorsal wall of the primary atrial segment. This dorsal mesenchymal protrusion is continuous with a mesenchymal cap on the leading edge of the primary atrial septum. Neither the mesenchymal tissues of the dorsal protrusion nor the mesenchymal cap on the edge of the primary septum expressed the endocardial tissue antigen recognized by 249-9G9 at any of the stages investigated. The developing pulmonary vein uses the dorsal mesocardium as a conduit to reach the primary atrial segment. Initially, the pulmonary pit, which will becomes the portal of entry for the pulmonary vein, is located along the midline, flanked by two myocardial ridges. As development progresses, tissue remodeling results in the incorporation of the portal of entry of the pulmonary vein in left atrial myocardium, which is recognized because of its high level of creatine. Closure of the primary atrial foramen by the primary atrial septum occurs as a consequence of the fusion of these mesenchymal structures.

摘要

利用一组先前描述的抗体,通过免疫组织化学方法研究了人类心脏心房腔的发育情况。这组抗体包括单克隆抗体249 - 9G9,它使我们能够区分心内膜垫来源的间充质组织与心外脏壁中胚层来源的间充质组织;还有一种识别肌酸激酶B同工型的单克隆抗体,它使我们能够区分右心房心肌和左心房心肌。用这些抗体获得的表达模式,结合从连续切片中获得的其他组织学信息,使我们能够详细描述从卡内基第14阶段开始的人类胚胎中,原始房间隔(原发隔)和肺静脉发育过程中涉及的形态发生事件。发现肌酸激酶B(CK - B)在左心房心肌中的表达水平始终高于右心房,在原发隔和左静脉瓣之间存在高表达和低表达的明显界限,这表明原发隔是左心房基因表达域的一部分。CK - B的这种表达模式让人联想到同源盒基因Pitx2的表达模式,最近已证明该基因对小鼠的房间隔形成很重要。这项研究还证明了背侧心内膜在心脏发育中一个未被充分认识的作用。从最早研究的阶段开始,背侧心内膜的间充质就突出到原始心房段的后壁。这种背侧间充质突出与原始房间隔前缘的间充质帽相连。在任何研究阶段,背侧突出的间充质组织和原始隔边缘的间充质帽都不表达249 - 9G9识别的心内膜组织抗原。发育中的肺静脉利用背侧心内膜作为通道到达原始心房段。最初,将成为肺静脉入口的肺凹位于中线,两侧有两个心肌嵴。随着发育的进行,组织重塑导致肺静脉入口并入左心房心肌,由于其高肌酸水平而被识别。原始房间隔关闭原始房间孔是这些间充质结构融合的结果。

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