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内源性逆转录病毒基因、疱疹病毒与多发性硬化症中的性别因素

Endogenous retroviral genes, Herpesviruses and gender in Multiple Sclerosis.

作者信息

Perron Hervé, Bernard Corinne, Bertrand Jean-Baptiste, Lang Alois B, Popa Iuliana, Sanhadji Kamel, Portoukalian Jacques

机构信息

GeNeuro, 14 Chemin des Aulx, CH-1228 Plan-Les Ouates, Geneva, Switzerland.

出版信息

J Neurol Sci. 2009 Nov 15;286(1-2):65-72. doi: 10.1016/j.jns.2009.04.034. Epub 2009 May 17.

Abstract

Unexpected findings on endogenous retroviral elements expressed in cells from patients with Multiple Sclerosis appear to open a new avenue of research, after years of research dedicated to the understanding of their biological significance in human health and disease. Human endogenous retroviral family W (HERV-W) RNA present in circulating viral particles (Multiple Sclerosis associated RetroViral element, MSRV) has been associated with the evolution and prognosis of Multiple Sclerosis. HERV-W elements encode a powerful immunopathogenic envelope protein (ENV) that activates a pro-inflammatory and autoimmune cascade through interaction with Toll-Like Receptor 4 (TLR4) on antigen-presenting cells, and triggers superantigen-like dysregulation of T-lymphocytes. HERV-W/ENV antigen has further been shown to be an upstream inducer of immunopathogenicity like that in MS and has repeatedly been detected in association with MS lesions in post-mortem brain studies. ENV protein now represents a novel target in MS, in our ongoing development of a neutralising therapeutic antibody. We here review the pieces of a puzzle, which now offer a consistent picture for Multiple Sclerosis aetiopathogenesis. Interestingly, at the gene-environment interface, this picture also includes gender-related specificities through the potential interplay with endogenous retrovirus type W copies present on the X chromosome.

摘要

在致力于理解内源性逆转录病毒元件在人类健康和疾病中的生物学意义的多年研究之后,多发性硬化症患者细胞中表达的内源性逆转录病毒元件的意外发现似乎开辟了一条新的研究途径。循环病毒颗粒中存在的人类内源性逆转录病毒W家族(HERV-W)RNA(多发性硬化症相关逆转录病毒元件,MSRV)与多发性硬化症的进展和预后相关。HERV-W元件编码一种强大的免疫致病包膜蛋白(ENV),该蛋白通过与抗原呈递细胞上的Toll样受体4(TLR4)相互作用激活促炎和自身免疫级联反应,并触发T淋巴细胞的超抗原样失调。HERV-W/ENV抗原进一步被证明是MS中免疫致病性的上游诱导物,并且在死后大脑研究中多次被检测到与MS病变相关。在我们正在进行的中和治疗性抗体的开发中,ENV蛋白现在代表了MS中的一个新靶点。我们在此回顾了这些拼图碎片,它们现在为多发性硬化症的病因发病机制提供了一幅连贯的图景。有趣的是,在基因-环境界面,这幅图景还包括通过与X染色体上存在的W型内源性逆转录病毒拷贝的潜在相互作用而产生的性别相关特异性。

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