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发育中和移植后的人类心脏中神经细胞黏附分子(N-CAM)的心肌定位及亚型

Myocardial localization and isoforms of neural cell adhesion molecule (N-CAM) in the developing and transplanted human heart.

作者信息

Gordon L, Wharton J, Moore S E, Walsh F S, Moscoso J G, Penketh R, Wallwork J, Taylor K M, Yacoub M H, Polak J M

机构信息

Department of Histochemistry, Royal Postgraduate Medical School, London, United Kingdom.

出版信息

J Clin Invest. 1990 Oct;86(4):1293-300. doi: 10.1172/JCI114837.

DOI:10.1172/JCI114837
PMID:2212013
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC296861/
Abstract

Neural cell adhesion molecule (N-CAM) has been implicated in cellular interactions involved in cardiac morphogenesis and innervation. Immunohistochemical techniques and Western blot analysis were used to determine the localization and isoforms of N-CAM in the developing and extrinsically denervated human heart. Myocardial and conducting cells in the fetal heart (7-24 wk gestation) exhibited sarcolemmal immunoreactivity, the major desialo N-CAM isoforms being 150, 145, 120, 115, and 110 kD. N-CAM expression appeared to be downregulated in the myocardium during adult life, with relatively little sarcolemmal immunoreactivity being detected in normal donor tissues. In contrast to the temporal changes observed in the myocardium, both the developing and mature cardiac innervation displayed N-CAM immunofluorescence staining, localized to neuronal cell bodies, nerve fascicles and fibres. Extrinsically denervated cardiac allografts, obtained 2 d to 91 mo after transplantation, showed extensive sarcolemmal and intercalated disc immunostaining and expression of 125-, 120-, and 115-kD isoforms. Tissues from explanted recipient hearts and atrial appendage samples obtained during coronary bypass graft operations were also examined and displayed varying amounts of N-CAM immunoreactivity. We conclude that the expression of N-CAM immunoreactivity and isoforms in the human heart is developmentally regulated and may be modulated by factors such as cardiac innervation and myocardial hypertrophy.

摘要

神经细胞黏附分子(N-CAM)与心脏形态发生和神经支配过程中的细胞相互作用有关。采用免疫组织化学技术和蛋白质印迹分析来确定N-CAM在发育中的和外在去神经支配的人类心脏中的定位和异构体。胎儿心脏(妊娠7-24周)中的心肌细胞和传导细胞表现出肌膜免疫反应性,主要的去唾液酸N-CAM异构体为150、145、120、115和110kD。在成年期,心肌中的N-CAM表达似乎下调,在正常供体组织中检测到的肌膜免疫反应性相对较少。与心肌中观察到的时间变化相反,发育中的和成熟的心脏神经支配均显示N-CAM免疫荧光染色,定位于神经元细胞体、神经束和纤维。移植后2天至91个月获得的外在去神经支配的心脏同种异体移植物显示广泛的肌膜和闰盘免疫染色以及125、120和115kD异构体的表达。还检查了来自移植受体心脏的组织和冠状动脉搭桥手术期间获得的心房附件样本,它们显示出不同程度的N-CAM免疫反应性。我们得出结论,人类心脏中N-CAM免疫反应性和异构体的表达受发育调控,并且可能受心脏神经支配和心肌肥大等因素的调节。

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