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替代轻链成分λ5的独特区域是前体B细胞受体信号传导的重链特异性调节因子。

The unique region of surrogate light chain component lambda5 is a heavy chain-specific regulator of precursor B cell receptor signaling.

作者信息

Guloglu F Betul, Bajor Ewa, Smith Brendan P, Roman Christopher A J

机构信息

Department of Microbiology and Immunology, School of Graduate Studies, State University of New York, Downstate Medical Center at Brooklyn, Brooklyn, NY 11203, USA.

出版信息

J Immunol. 2005 Jul 1;175(1):358-66. doi: 10.4049/jimmunol.175.1.358.

Abstract

Signals transduced by precursor-BCRs (pre-BCRs) composed of Ig mu heavy chains (HCs) and the surrogate L chain components lambda5 and VpreB are critical for B cell development. A conserved unique region (UR) of lambda5 was shown to activate pre-BCR complexes in transformed cells and to engage putative ligands, but its contribution to pre-B cell development is not known. It is also not clear why the lambda-like sequences in lambda5 are used to select HCs that will associate mainly with kappa L chains. In this study, we show that, in transformed and primary mouse B cell progenitors, receptors containing full-length HCs and lacking the lambda5UR were expressed at higher surface levels, but exhibited reduced activity compared with normal pre-BCRs in supporting developmental changes that accompany the progenitor to pre-B cell transition in primary cell culture systems and in the bone marrow in vivo. In contrast, deletion of the lambda5UR did not change net signaling output by the Dmu-pre-BCR, a developmentally defective receptor that exhibited impaired activity in the primary cell culture system. Moreover, the lambda-like sequences in lambda5 were more accommodating than kappa in supporting surface expression and signaling by the different HCs. These results show that the lambda5UR is important, although not essential, for surrogate L chain-dependent receptor signaling in primary cells, and furthermore may help allow discrimination of signaling competency between normal and Dmu-pre-BCRs. That the lambda-like portion of lambda5 in the absence of the UR was nondiscriminatory suggests that the lambda5UR focuses pre-BCR-dependent selection on the HC V region.

摘要

由免疫球蛋白μ重链(HCs)以及替代轻链成分λ5和VpreB组成的前B细胞受体(pre-BCRs)转导的信号对于B细胞发育至关重要。λ5的一个保守独特区域(UR)已被证明可在转化细胞中激活pre-BCR复合物并与假定的配体结合,但其对前B细胞发育的贡献尚不清楚。同样不清楚的是,为何λ5中的类λ序列用于选择主要与κ轻链结合的HCs。在本研究中,我们发现,在转化的和原代小鼠B细胞祖细胞中,含有全长HCs且缺乏λ5UR的受体在表面表达水平更高,但与正常pre-BCRs相比,在支持原代细胞培养系统和体内骨髓中祖细胞向前B细胞转变所伴随的发育变化方面,其活性降低。相反,λ5UR的缺失并未改变Dmu-pre-BCR的净信号输出,Dmu-pre-BCR是一种在原代细胞培养系统中活性受损的发育缺陷型受体。此外,λ5中的类λ序列在支持不同HCs的表面表达和信号传导方面比κ更具适应性。这些结果表明,λ5UR对于原代细胞中依赖替代轻链的受体信号传导很重要,尽管不是必需的,而且还可能有助于区分正常pre-BCR和Dmu-pre-BCR之间的信号传导能力。在没有UR的情况下,λ5的类λ部分没有区分性,这表明λ5UR将pre-BCR依赖的选择集中在HC V区域。

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