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鉴定髓鞘再生天然抗体的方法。

Method of identifying natural antibodies for remyelination.

机构信息

Department of Neurology, Guggenheim 401, Mayo Clinic, Rochester, MN 55905, USA.

出版信息

J Clin Immunol. 2010 May;30 Suppl 1(0 1):S50-5. doi: 10.1007/s10875-010-9406-5.

Abstract

INTRODUCTION

Natural autoantibodies are part of the normal human immunoglobulin repertoire. These antibodies react to self-antigens, are usually polyreactive with relatively low affinity, and typically are of the IgM isotype. Natural IgMs in mice that stimulated remyelination in central nervous system (CNS) demyelinating disease all shared the characteristics of binding to the surface of live oligodendrocytes and myelinated tracts in living slices of CNS tissue.

METHODS

A screen for human IgMs with similar character resulted in two human natural antibodies, which when injected peripherally into animal models of demyelination induced remyelination. A recombinant human IgM (rHIgM22) that also promoted remyelination in vivo was constructed.

RESULTS

Very small doses of this IgM are required for the promotion of remyelination (EC50 is 460 ng per 20-g mouse). It is clear that after peripheral delivery, rHIgM22 enters the CNS and accumulates in CNS lesions. rHIgM22 was tracked in living mice using ferritin-labeled antihuman mu chain antibodies visualized by magnetic resonance imaging and traditional immunocytochemistry. Although the exact antigen recognized by rHIgM22 is not known, all mouse IgMs that promote remyelination bind to myelin membrane lipids, suggesting the antigen for rHIgM22 is similar.

CONCLUSIONS

We propose that the IgMs bind to CNS cells and reorganize the membrane, initiating a signal that results in oligodendrocyte proliferation and/or protection with an end result of increased myelin. Recombinant natural human antibodies are potentially important therapeutic molecules that may modulate a wide spectrum of human disease.

摘要

简介

天然自身抗体是正常人类免疫球蛋白库的一部分。这些抗体针对自身抗原反应,通常具有多反应性和相对较低的亲和力,并且通常为 IgM 同种型。在中枢神经系统(CNS)脱髓鞘疾病中刺激髓鞘再生的小鼠天然 IgM 均具有与活少突胶质细胞表面结合的特征,并且在活的 CNS 组织切片中与有髓神经纤维结合。

方法

筛选具有类似特征的人 IgM 导致了两种人天然抗体,当将其外周注射到脱髓鞘动物模型中时,会诱导髓鞘再生。构建了一种能够在体内促进髓鞘再生的重组人 IgM(rHIgM22)。

结果

这种 IgM 促进髓鞘再生所需的剂量非常小(EC50 为每 20 克小鼠 460 纳克)。很明显,在周围给药后,rHIgM22 进入 CNS 并在 CNS 病变中积聚。使用铁蛋白标记的抗人 mu 链抗体通过磁共振成像和传统免疫细胞化学在活小鼠中追踪 rHIgM22。尽管尚不清楚 rHIgM22 识别的确切抗原,但所有促进髓鞘再生的小鼠 IgM 均与髓鞘膜脂质结合,这表明 rHIgM22 的抗原相似。

结论

我们提出 IgM 结合到 CNS 细胞并重组膜,引发导致少突胶质细胞增殖和/或保护的信号,最终导致髓鞘增加。重组天然人抗体可能是潜在的重要治疗分子,可调节广泛的人类疾病。

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