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在以 IgM 为主导的 repertoire 中存在针对 BK 多瘤病毒的广泛中和 IgG。

A cluster of broadly neutralizing IgG against BK polyomavirus in a repertoire dominated by IgM.

机构信息

Nantes Universitéhttps://ror.org/05c1qsg97 , CHU Nantes, INSERM, Center for Research in Transplantation and Translational Immunology, UMR 1064, ITUN, Nantes, France.

Nantes Université, Inserm UMR 1307, CNRS UMR 6075, Université d'Angers, CRCI2NA, Nantes, France.

出版信息

Life Sci Alliance. 2023 Jan 30;6(4). doi: 10.26508/lsa.202201567. Print 2023 Apr.

Abstract

The BK polyomavirus (BKPyV) is an opportunistic pathogen, which is only pathogenic in immunosuppressed individuals, such as kidney transplant recipients, in whom BKPyV can cause significant morbidity. To identify broadly neutralizing antibodies against this virus, we used fluorescence-labeled BKPyV virus-like particles to sort BKPyV-specific B cells from the PBMC of KTx recipients, then single-cell RNAseq to obtain paired heavy- and light-chain antibody sequences from 2,106 sorted B cells. The BKPyV-specific repertoire was highly diverse in terms of both V-gene usage and clonotype diversity and included most of the IgM B cells, including many with extensive somatic hypermutation. In two patients where sufficient data were available, IgM B cells in the BKPyV-specific dataset had significant differences in V-gene usage compared with IgG B cells from the same patient. CDR3 sequence-based clustering allowed us to identify and characterize three broadly neutralizing "41F17-like" clonotypes that were predominantly IgG, suggesting that some specific BKPyV capsid epitopes are preferentially targeted by IgG.

摘要

BK 多瘤病毒(BKPyV)是一种机会性病原体,仅在免疫抑制个体中具有致病性,例如肾移植受者,其中 BKPyV 可导致严重的发病率。为了鉴定针对该病毒的广泛中和抗体,我们使用荧光标记的 BKPyV 病毒样颗粒从 KTx 受者的 PBMC 中分离 BKPyV 特异性 B 细胞,然后进行单细胞 RNAseq,从 2106 个分离的 B 细胞中获得配对的重链和轻链抗体序列。BKPyV 特异性库在 V 基因使用和克隆型多样性方面具有高度多样性,包括大多数 IgM B 细胞,其中许多具有广泛的体细胞超突变。在两名患者中,提供了足够的数据,与来自同一患者的 IgG B 细胞相比,BKPyV 特异性数据集的 IgM B 细胞在 V 基因使用方面存在显着差异。基于 CDR3 序列的聚类允许我们鉴定和表征三个广泛中和的“41F17 样”克隆型,主要是 IgG,这表明一些特定的 BKPyV 衣壳表位优先被 IgG 靶向。

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