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自身反应性B细胞受体模拟自主前B细胞受体信号传导并诱导早期B细胞增殖。

Autoreactive B cell receptors mimic autonomous pre-B cell receptor signaling and induce proliferation of early B cells.

作者信息

Köhler Fabian, Hug Eva, Eschbach Cathrin, Meixlsperger Sonja, Hobeika Elias, Kofer Juliane, Wardemann Hedda, Jumaa Hassan

机构信息

Department of Molecular Immunology, Faculty of Biology and Centre for Biological Signalling Studies (bioss), Albert-Ludwigs-University and Max-Planck-Institute for Immunobiology, 79108 Freiburg, Germany.

出版信息

Immunity. 2008 Dec 19;29(6):912-21. doi: 10.1016/j.immuni.2008.10.013. Epub 2008 Dec 11.

Abstract

The majority of early immature B cells express autoreactive B cell receptors (BCRs) that are, according to the current view, negatively selected to avoid the production of self-reactive antibodies. Here, we show that polyreactive BCRs, which recognize multiple self-antigens, induced autonomous signaling and selective expansion of B cell precursors in a manner comparable to the pre-BCR. We found that the pre-BCR was capable of recognizing multiple self-antigens and that a signaling-deficient pre-BCR lacking the non-Ig region of the surrogate-light-chain component lambda5 was rescued by the complementarity-determining region 3 derived from heavy chains of polyreactive receptors. Importantly, bone marrow B cells from mice carrying Ig transgenes for an autoreactive BCR showed increased cell-cycle activity, which could not be detected in cells lacking the transgenic BCR. Together, the pre-BCR has evolved to ensure self-recognition because autoreactivity is required for positive selection of B cell precursors.

摘要

大多数早期未成熟B细胞表达自身反应性B细胞受体(BCR),根据目前的观点,这些受体经过阴性选择以避免产生自身反应性抗体。在此,我们表明,识别多种自身抗原的多反应性BCR以类似于前BCR的方式诱导B细胞前体的自主信号传导和选择性扩增。我们发现前BCR能够识别多种自身抗原,并且缺乏替代轻链成分lambda5非Ig区域的信号缺陷型前BCR可由多反应性受体重链衍生的互补决定区3挽救。重要的是,携带自身反应性BCR的Ig转基因小鼠的骨髓B细胞显示出增加的细胞周期活性,而在缺乏转基因BCR的细胞中未检测到这种活性。总之,前BCR已经进化以确保自身识别,因为自身反应性是B细胞前体阳性选择所必需的。

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