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新冠病毒感染中浆母细胞和自身反应性B细胞的成熟轨迹及转录图谱

Maturation trajectories and transcriptional landscape of plasmablasts and autoreactive B cells in COVID-19.

作者信息

Schultheiß Christoph, Paschold Lisa, Willscher Edith, Simnica Donjete, Wöstemeier Anna, Muscate Franziska, Wass Maxi, Eisenmann Stephan, Dutzmann Jochen, Keyßer Gernot, Gagliani Nicola, Binder Mascha

机构信息

Department of Internal Medicine IV, Oncology/Hematology, Martin-Luther-University Halle-Wittenberg, Ernst-Grube-Straße 40, 06120 Halle (Saale), Germany.

I. Department of Medicine and Department for General, Visceral and Thoracic Surgery, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.

出版信息

iScience. 2021 Nov 19;24(11):103325. doi: 10.1016/j.isci.2021.103325. Epub 2021 Oct 23.

Abstract

In parasite and viral infections, aberrant B cell responses can suppress germinal center reactions thereby blunting long-lived memory and may provoke immunopathology including autoimmunity. Using COVID-19 as model, we set out to identify serological, cellular, and transcriptomic imprints of pathological responses linked to autoreactive B cells at single-cell resolution. We show that excessive plasmablast expansions are prognostically adverse and correlate with autoantibody production but do not hinder the formation of neutralizing antibodies. Although plasmablasts followed interleukin-4 (IL-4) and BAFF-driven developmental trajectories, were polyclonal, and not enriched in autoreactive B cells, we identified two memory populations (CD80/ISG15 and CD11c/SOX5/T-bet) with immunogenetic and transcriptional signs of autoreactivity that may be the cellular source of autoantibodies in COVID-19 and that may persist beyond recovery. Immunomodulatory interventions discouraging such adverse responses may be useful in selected patients to shift the balance from autoreactivity toward long-term memory.

摘要

在寄生虫和病毒感染中,异常的B细胞反应可抑制生发中心反应,从而削弱长期记忆,并可能引发包括自身免疫在内的免疫病理反应。以新冠病毒病(COVID-19)为模型,我们着手以单细胞分辨率鉴定与自身反应性B细胞相关的病理反应的血清学、细胞和转录组印记。我们发现,浆母细胞过度扩增在预后方面不利,且与自身抗体产生相关,但并不妨碍中和抗体的形成。尽管浆母细胞遵循白细胞介素-4(IL-4)和B细胞激活因子(BAFF)驱动的发育轨迹,具有多克隆性,且自身反应性B细胞未富集,但我们鉴定出了两个具有自身反应性免疫遗传学和转录特征的记忆群体(CD80/ISG15和CD11c/SOX5/T-bet),它们可能是COVID-19中自身抗体的细胞来源,并且可能在康复后仍持续存在。抑制此类不良反应的免疫调节干预措施可能对特定患者有用,以将平衡从自身反应性转向长期记忆。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/703e/8586746/6d135a7adc72/fx1.jpg

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