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儿童多发性硬化症中针对髓鞘表面抗原的年龄依赖性B细胞自身免疫。

Age-dependent B cell autoimmunity to a myelin surface antigen in pediatric multiple sclerosis.

作者信息

McLaughlin Katherine A, Chitnis Tanuja, Newcombe Jia, Franz Bettina, Kennedy Julia, McArdel Shannon, Kuhle Jens, Kappos Ludwig, Rostasy Kevin, Pohl Daniela, Gagne Donald, Ness Jayne M, Tenembaum Silvia, O'Connor Kevin C, Viglietta Vissia, Wong Susan J, Tavakoli Norma P, de Seze Jerome, Idrissova Zhannat, Khoury Samia J, Bar-Or Amit, Hafler David A, Banwell Brenda, Wucherpfennig Kai W

机构信息

Department of Cancer Immunology and AIDS, Dana-Farber Cancer Institute, Brigham and Women's Hospital, Boston, MA 02115, USA.

出版信息

J Immunol. 2009 Sep 15;183(6):4067-76. doi: 10.4049/jimmunol.0801888. Epub 2009 Aug 17.

Abstract

Multiple sclerosis (MS) typically manifests in early to mid adulthood, but there is increasing recognition of pediatric-onset MS, aided by improvements in imaging techniques. The immunological mechanisms of disease are largely unexplored in pediatric-onset MS, in part because studies have historically focused on adult-onset disease. We investigated autoantibodies to myelin surface Ags in a large cohort of pediatric MS cases by flow cytometric labeling of transfectants that expressed different myelin proteins. Although Abs to native myelin oligodendrocyte glycoprotein (MOG) were uncommon among adult-onset patients, a subset of pediatric patients had serum Abs that brightly labeled the MOG transfectant. Abs to two other myelin surface Ags were largely absent. Affinity purification of MOG Abs as well as competition of binding with soluble MOG documented their binding specificity. Such affinity purified Abs labeled myelin and glial cells in human CNS white matter as well as myelinated axons in gray matter. The prevalence of such autoantibodies was highest among patients with a very early onset of MS: 38.7% of patients less than 10 years of age at disease onset had MOG Abs, compared with 14.7% of patients in the 10- to 18-year age group. B cell autoimmunity to this myelin surface Ag is therefore most common in patients with a very early onset of MS.

摘要

多发性硬化症(MS)通常在成年早期至中期出现,但随着成像技术的改进,儿童期发病的MS越来越受到关注。儿童期发病的MS的免疫机制在很大程度上尚未得到探索,部分原因是历史上的研究主要集中在成年期发病的疾病上。我们通过对表达不同髓鞘蛋白的转染子进行流式细胞术标记,在一大群儿童MS病例中研究了针对髓鞘表面抗原的自身抗体。虽然在成年期发病的患者中,针对天然髓鞘少突胶质细胞糖蛋白(MOG)的抗体并不常见,但一部分儿童患者的血清抗体能强烈标记MOG转染子。针对其他两种髓鞘表面抗原的抗体基本不存在。对MOG抗体进行亲和纯化以及与可溶性MOG的结合竞争证明了它们的结合特异性。这种亲和纯化的抗体标记了人类中枢神经系统白质中的髓鞘和神经胶质细胞以及灰质中的有髓轴突。这种自身抗体的患病率在MS发病非常早的患者中最高:疾病发作时年龄小于10岁的患者中有38.7%有MOG抗体,而10至18岁年龄组的患者中这一比例为14.7%。因此,针对这种髓鞘表面抗原的B细胞自身免疫在MS发病非常早的患者中最为常见。

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