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抗DNA抗体转基因C57BL/6和BALB/c小鼠外周B细胞中的等位基因和同种型轻链包涵体。

Allelic and isotypic light chain inclusion in peripheral B cells from anti-DNA antibody transgenic C57BL/6 and BALB/c mice.

作者信息

Witsch Esther J, Bettelheim Eldad

机构信息

Department of Pathology, Gwen Knapp Center for Lupus and Immunology Research, University of Chicago, Chicago, IL 60637, USA.

出版信息

J Immunol. 2008 Mar 15;180(6):3708-18. doi: 10.4049/jimmunol.180.6.3708.

DOI:10.4049/jimmunol.180.6.3708
PMID:18322176
Abstract

Most mature B lymphocytes express one BCR L chain, kappa or lambda, but recent work has shown that there are exceptions in that some B lymphocytes express both kappa and lambda and some even bear two different kappa L chains. Using the anti-DNA H chain-transgenic mouse, 56R, we find that B cells with pre-existing autoreactivity are especially subject to L chain inclusion. Specifically, we show that isotypic and allelic inclusion enables autoreactive B cells to bypass central tolerance giving rise to B cells that retain dangerous features. One receptor in dual receptor B cells is an editor L chain, i.e., neutralizes or alters self-reactivity of the 56R H chain transgene. We compare the 56R mouse when on the C57/BL/6 background, a strain prone to autoimmunity, with that of 56R when on the BALB/c background, a strain that resists autoimmunity. In the B6.56R mouse, polyreactive B cells with dual L chain move to the follicular B cell compartment. Their localization in the follicular compartment may explain the ease with which B cells in the B6.56R differentiate into autoantibody-producing plasma cells. Likewise, in the BALB/c.56R mouse, dual L chain B cells are found in the follicular B cell compartment. Yet, the lack of autoantibody-producing plasma cells in the BALB/c.56R suggests that postfollicular tolerance checkpoints are intact. The Jkappa usage in dual kappa L chain B cells suggests increased receptor editing activity and is consistent with the expected distribution of Jkappa genes in our computational model for random selection of Jkappa.

摘要

大多数成熟的B淋巴细胞表达一种BCR轻链,κ链或λ链,但最近的研究表明也有例外,即一些B淋巴细胞同时表达κ链和λ链,甚至有些带有两种不同的κ轻链。利用抗DNA重链转基因小鼠56R,我们发现预先存在自身反应性的B细胞特别容易出现轻链包含现象。具体而言,我们表明同种型和等位基因包含使自身反应性B细胞能够绕过中枢耐受,从而产生保留危险特征的B细胞。双受体B细胞中的一种受体是编辑轻链,即中和或改变56R重链转基因的自身反应性。我们比较了处于易患自身免疫的C57/BL/6背景下的56R小鼠和处于抵抗自身免疫的BALB/c背景下的56R小鼠。在B6.56R小鼠中,具有双轻链的多反应性B细胞迁移到滤泡B细胞区室。它们在滤泡区室中的定位可能解释了B6.56R小鼠中的B细胞易于分化为产生自身抗体的浆细胞的原因。同样,在BALB/c.56R小鼠中,在滤泡B细胞区室中发现了双轻链B细胞。然而,BALB/c.56R小鼠中缺乏产生自身抗体的浆细胞表明滤泡后耐受检查点是完整的。双κ轻链B细胞中Jκ的使用表明受体编辑活性增加,并且与我们用于随机选择Jκ的计算模型中Jκ基因的预期分布一致。

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