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首页> 外文期刊>Immunobiology: Zeitschrift fur Immunitatsforschung >Role of β 1-adrenoceptor autoantibodies in the pathogenesis of dilated cardiomyopathy
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Role of β 1-adrenoceptor autoantibodies in the pathogenesis of dilated cardiomyopathy

机译:β1肾上腺素受体自身抗体在扩张型心肌病发病机制中的作用

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摘要

Dilated cardiomyopathy (DCM) is a common cause of heart failure. After the identification of several immune regulatory abnormalities in DCM increasing attention has been focused on autoimmune mechanisms as potential key elements in the pathogenesis of the disease. DCM has appeared to be often related to elevated levels of autoantibodies against cardiac structural or functional proteins. Among several autoantibodies (AABs) which react against cardiac cellular proteins that have been detected in sera from DCM patients, those against β1-adrenoreceptors (β1-ARs) appeared particularly relevant from a pathophysiological point of view. The available experimental and clinical data suggest that in β1-AAB-positive patients with DCM the cardiomyopathy might be a β1-AR-targeted autoimmune disease. This review summarizes the present knowledge about β1-AABs, their role in DCM etiopathogenesis and the therapeutic benefits of β1-AAB removal. Special attention is focused on the possible origin of β1-AABs, their interaction with the β 1-ARs, the prevalence of β1-AABs in patients with DCM and the potential pathophysiologic impact of these AABs in the development and progression of the disease. Attention is also given to the amelioration of β1-AAB cardiotoxicity by β 1-AR antagonists and especially to immunoadsorption (IA) therapy. Responsiveness to IA therapy and its long-term efficiency, as well as post-IA reappearance of β 1-AABs and its impact on patients' outcome are also discussed in detail. Finally the important question of whether the therapeutic results of IA are indeed related to β 1-AAB removal is analyzed on the basis of available data. Overall the review aims to provide an exhaustive overview of the available experimental and clinical data on β 1-AABs in DCM and also a theoretical and practical basis for clinicians who are or intend in future to be engaged in this field.
机译:扩张型心肌病(DCM)是心力衰竭的常见原因。在确定DCM中的几种免疫调节异常后,人们越来越关注自身免疫机制,将其作为疾病发病机理中的潜在关键要素。 DCM似乎经常与针对心脏结构或功能蛋白的自身抗体水平升高有关。从病理生理学角度来看,在几种抗DCM患者血清中检测到的心脏细胞蛋白发生反应的自身抗体(AAB)中,针对β1-肾上腺素能受体(β1-ARs)的那些自身抗体显得尤为重要。现有的实验和临床数据表明,在β1-AAB阳性的DCM患者中,心肌病可能是针对β1-AR的自身免疫性疾病。这篇综述总结了有关β1-AABs,它们在DCM发病机制中的作用以及去除β1-AAB的治疗益处的现有知识。特别关注的是β1-AAB的可能来源,它们与β1-AR的相互作用,DCM患者中β1-AAB的患病率以及这些AAB在疾病发展和进程中的潜在病理生理影响。也关注通过β1-AR拮抗剂改善β1-AAB的心脏毒性,尤其是免疫吸附(IA)疗法。还详细讨论了对IA治疗的反应性,其长期有效性以及IA后β1-AAB的重新出现及其对患者预后的影响。最后,根据现有数据分析了IA的治疗结果是否确实与β1-AAB去除有关的重要问题。总体而言,本综述旨在详尽地概述DCM中β1-AAB的可用实验和临床数据,并为有意或将来打算从事该领域的临床医生提供理论和实践基础。

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