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风湿性心脏病与黏液瘤样变性:自身免疫反应和基质紊乱导致的瓣膜损害的差异与相似之处。

Rheumatic Heart Disease and Myxomatous Degeneration: Differences and Similarities of Valve Damage Resulting from Autoimmune Reactions and Matrix Disorganization.

作者信息

Martins Carlo de Oliveira, Demarchi Lea, Ferreira Frederico Moraes, Pomerantzeff Pablo Maria Alberto, Brandao Carlos, Sampaio Roney Orismar, Spina Guilherme Sobreira, Kalil Jorge, Cunha-Neto Edecio, Guilherme Luiza

机构信息

Heart Institute (InCor), School of Medicine, University of São Paulo, São Paulo, São Paulo, Brazil.

Institute of Investigation in Immunology, National Institute for Science and Technology, University of São Paulo, São Paulo, São Paulo, Brazil.

出版信息

PLoS One. 2017 Jan 25;12(1):e0170191. doi: 10.1371/journal.pone.0170191. eCollection 2017.

Abstract

Autoimmune inflammatory reactions leading to rheumatic fever (RF) and rheumatic heart disease (RHD) result from untreated Streptococcus pyogenes throat infections in individuals who exhibit genetic susceptibility. Immune effector mechanisms have been described that lead to heart tissue damage culminating in mitral and aortic valve dysfunctions. In myxomatous valve degeneration (MXD), the mitral valve is also damaged due to non-inflammatory mechanisms. Both diseases are characterized by structural valve disarray and a previous proteomic analysis of them has disclosed a distinct profile of matrix/structural proteins differentially expressed. Given their relevance in organizing valve tissue, we quantitatively evaluated the expression of vimentin, collagen VI, lumican, and vitronectin as well as performed immunohistochemical analysis of their distribution in valve tissue lesions of patients in both diseases. We identified abundant expression of two isoforms of vimentin (45 kDa, 42 kDa) with reduced expression of the full-size protein (54 kDa) in RHD valves. We also found increased vitronectin expression, reduced collagen VI expression and similar lumican expression between RHD and MXD valves. Immunohistochemical analysis indicated disrupted patterns of these proteins in myxomatous degeneration valves and disorganized distribution in rheumatic heart disease valves that correlated with clinical manifestations such as valve regurgitation or stenosis. Confocal microscopy analysis revealed a diverse pattern of distribution of collagen VI and lumican into RHD and MXD valves. Altogether, these results demonstrated distinct patterns of altered valve expression and tissue distribution/organization of structural/matrix proteins that play important pathophysiological roles in both valve diseases.

摘要

导致风湿热(RF)和风湿性心脏病(RHD)的自身免疫性炎症反应,是由未治疗的化脓性链球菌咽喉感染引起的,这些感染发生在具有遗传易感性的个体中。已经描述了导致心脏组织损伤最终导致二尖瓣和主动脉瓣功能障碍的免疫效应机制。在黏液瘤样瓣膜变性(MXD)中,二尖瓣也因非炎症机制而受损。这两种疾病的特征都是瓣膜结构紊乱,之前对它们的蛋白质组学分析揭示了差异表达的基质/结构蛋白的独特谱。鉴于它们在组织瓣膜组织中的相关性,我们定量评估了波形蛋白、胶原蛋白VI、核纤层蛋白和玻连蛋白的表达,并对它们在这两种疾病患者瓣膜组织病变中的分布进行了免疫组织化学分析。我们发现在RHD瓣膜中波形蛋白的两种异构体(45 kDa、42 kDa)表达丰富,而全长蛋白(54 kDa)表达减少。我们还发现RHD和MXD瓣膜之间玻连蛋白表达增加、胶原蛋白VI表达减少且核纤层蛋白表达相似。免疫组织化学分析表明,这些蛋白质在黏液瘤样变性瓣膜中的模式被破坏,在风湿性心脏病瓣膜中分布紊乱,这与瓣膜反流或狭窄等临床表现相关。共聚焦显微镜分析揭示了胶原蛋白VI和核纤层蛋白在RHD和MXD瓣膜中的不同分布模式。总之,这些结果表明,在这两种瓣膜疾病中,结构/基质蛋白的瓣膜表达改变以及组织分布/组织化存在不同模式,这些模式发挥着重要的病理生理作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4259/5266332/a1b87a1130fe/pone.0170191.g001.jpg

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