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人类心脏中细胞凋亡的正常与异常后果:从出生后形态发生到阵发性心律失常。

Normal and abnormal consequences of apoptosis in the human heart: from postnatal morphogenesis to paroxysmal arrhythmias.

作者信息

James T N

机构信息

Department of Medicine, University of Texas Medical Branch, Galveston 77555-0129.

出版信息

Trans Am Clin Climatol Assoc. 1994;105:145-77; discussion 177-8.

Abstract

Apoptosis and necrosis are two distinctly different forms of cell death and both occur in the human heart. In contrast to necrosis, apoptosis is not associated with inflammation and there are two reasons for this. The apoptotic cell does not swell or rupture prior to its being engulfed by either a macrophage or even a neighboring like cell. And the phagocytosis occurs with unusual rapidity. Apoptosis, also thought of as cell suicide, is a tidy way of removing cells no longer useful, in essence a form of selective deletion. These features make apoptosis a valuable component of morphogenesis, mediation of hormonal and immunological responses, and the homeostatic balance between hypertrophy and atrophy or involution. In the human heart apoptosis has been found in the sinus node of patients with the long QT syndrome. It most likely participates in the important postnatal morphogenesis of the sinus node, AV (atrioventricular) node and His bundle. Apoptosis may also participate in the genesis and pathophysiology of cardiomyopathy, paroxysmal arrhythmias or conduction disturbances (some of which may be responsible for sudden death), focal fibromuscular dysplasia of small coronary arteries, hereditary medial degeneration of the tunica media of coronary arteries, and arrhythmogenic right ventricular dysplasia. The possible role of apoptosis in numerous other changes in the human heart merit future investigation, among them being the pathogenesis of atherosclerosis and mechanisms of ageing in the myocardium.

摘要

凋亡和坏死是细胞死亡的两种截然不同的形式,二者均发生于人类心脏。与坏死不同,凋亡不伴有炎症反应,原因有二。凋亡细胞在被巨噬细胞或相邻同类细胞吞噬之前不会肿胀或破裂。而且吞噬作用发生得异常迅速。凋亡,也被认为是细胞自杀,是一种清除不再有用细胞的有序方式,本质上是一种选择性删除形式。这些特征使凋亡成为形态发生、激素和免疫反应调节以及肥大与萎缩或退化之间稳态平衡的重要组成部分。在人类心脏中,已在长QT综合征患者的窦房结中发现凋亡现象。它很可能参与窦房结、房室(AV)结和希氏束重要的出生后形态发生过程。凋亡也可能参与心肌病、阵发性心律失常或传导障碍(其中一些可能导致猝死)、小冠状动脉局灶性纤维肌发育不良、冠状动脉中膜遗传性中层退变以及致心律失常性右心室发育不良的发生和病理生理过程。凋亡在人类心脏众多其他变化中的可能作用值得未来研究,其中包括动脉粥样硬化的发病机制和心肌衰老机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/be8a/2376730/b1d659e33da2/tacca00083-0209-a.jpg

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