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纵向单细胞细胞因子反应揭示复发缓解型多发性硬化症患者反复出现的自身免疫性髓鞘反应性

Longitudinal single-cell cytokine responses reveal recurrent autoimmune myelin reactivity in relapsing--remitting multiple sclerosis patients.

作者信息

Moldovan I R, Rudick R A, Cotleur A C, Born S E, Lee J C, Karafa M T, Pelfrey C M

机构信息

Department of Neurosciences, Cleveland Clinic Foundation, Cleveland, OH 44195-0001, USA.

出版信息

Mult Scler. 2005 Jun;11(3):251-60. doi: 10.1191/1352458505ms1165oa.

Abstract

The relationship between multiple sclerosis (MS) disease activity and myelin protein-induced cytokine responses over time is not elucidated. We addressed this relationship by examining longitudinal cytokine responses to myelin proteins every three months for one year, in the context of gadolinium (gad)-enhancing brain lesions and of clinical relapses. The ELISPOT assay was used to determine the ex vivo cytokine production in response to nine amino acid long peptides spanning the entire proteolipid protein (PLP) and myelin basic protein (MBP) molecules in relapsing-remitting (RR) MS patients and matched healthy controls. We identified three longitudinal levels of myelin-induced cytokine secretion by adding up the positive responses for all PLP or MBP peptides obtained for five timepoints, at three-month intervals: low reactivity (< 200 cumulative cytokine-secreting cells), isolated peptide reactivity (201-450 cumulative cytokine-secreting cells) and recurrent protein-wide bursts of cytokine reactivity (> 451 cumulative cytokine-secreting cells). The majority of MS patients showed recurrent bursts to PLP and MBP. In contrast, controls showed a more even distribution between all levels of cytokine reactivity. The majority of patients with gad-enhancing lesions showed PLP/IFN gamma and MBP/IFN gamma recurrent burst responses. This is the first longitudinal study on MS patients in which nine amino acid long myelin peptides are used to reveal the broad range of PLP- and MBP-peptide cytokine reactivity across the whole molecule of these two major myelin proteins. This study also reveals the extremely dynamic nature of the immune reactivity to numerous regions of myelin, which can fluctuate dramatically over time. Such fluctuation could hamper the efficacy of antigen-based therapies for MS.

摘要

多发性硬化症(MS)疾病活动与髓磷脂蛋白诱导的细胞因子反应随时间的关系尚未阐明。我们通过在钆(gad)增强脑病变和临床复发的背景下,对复发缓解型(RR)MS患者和匹配的健康对照每三个月检测一次对髓磷脂蛋白的纵向细胞因子反应,来研究这种关系。ELISPOT试验用于确定复发缓解型MS患者和匹配的健康对照对跨越整个蛋白脂蛋白(PLP)和髓磷脂碱性蛋白(MBP)分子的九个氨基酸长肽的体外细胞因子产生情况。我们通过将每隔三个月的五个时间点获得的所有PLP或MBP肽的阳性反应相加,确定了髓磷脂诱导的细胞因子分泌的三个纵向水平:低反应性(<200个累积细胞因子分泌细胞)、孤立肽反应性(201 - 450个累积细胞因子分泌细胞)和细胞因子反应性的反复全蛋白爆发(>451个累积细胞因子分泌细胞)。大多数MS患者对PLP和MBP表现出反复爆发。相比之下,对照组在细胞因子反应性的所有水平之间分布更为均匀。大多数有钆增强病变的患者表现出PLP/IFNγ和MBP/IFNγ反复爆发反应。这是第一项针对MS患者的纵向研究,其中使用九个氨基酸长的髓磷脂肽来揭示这两种主要髓磷脂蛋白整个分子上广泛的PLP和MBP肽细胞因子反应性。这项研究还揭示了对髓磷脂众多区域的免疫反应性具有极强的动态性质,其可随时间发生显著波动。这种波动可能会妨碍基于抗原的MS治疗的疗效。

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