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登革热和 COVID-19 感染中增殖性浆母细胞的双面性。

The Janus face of proliferating plasmablasts in dengue and COVID-19 infections.

机构信息

Department of Bioengineering, University of California, San Diego, La Jolla, CA, United States.

Department of Cellular and Molecular Medicine, University of California, San Diego, La Jolla, CA, United States.

出版信息

Front Immunol. 2023 Aug 11;14:1068424. doi: 10.3389/fimmu.2023.1068424. eCollection 2023.

Abstract

INTRODUCTION

B cells play an integral role in the immune response to both dengue fever and COVID-19. Prior scRNAseq analyses of peripheral plasmablasts in COVID-19 have revealed a heterogeneous population with distinct cell subsets associated with proliferation; prior studies in patients with dengue fever have likewise shown the presence of proliferative pre-plasmablasts in the circulation. These findings may have implications for disease severity. In this study, we sought to gain a mechanistic understanding of the intracellular processes in naive and memory B cells that are associated with and may lead to an expanded proliferative plasmablast population in the circulation.

METHODS

We analyzed age-controlled (pediatric and adult), peripheral blood mononuclear cell scRNAseq datasets from patients infected with either dengue (primary or secondary) or COVID-19 (non-severe or severe) from previously published studies. Our preliminary analysis showed that pediatric patients with dengue and adults with COVID-19 had an expanded proliferative plasmablast (p-PB) population. By contrast, neither the adults with dengue nor the children with COVID-19 in our dataset had p-PBs. We used this distinctive preliminary signature to guide our analyses design and expanded our analyses to naive and memory B cells.

RESULTS

In age/disease conditions with and without p-PBs, we found differences in cell sensing and activation, including via the B cell receptor and downstream signal transduction. Likewise, inflammation was mediated differently: relative to groups without p-PBs, those with p-PBs had increased expression of interferon response and S100 genes (particularly severe COVID-19). Furthermore, several transcription factors at the nexus of activation, inflammation, and cell fate decisions were expressed differently in groups with and without p-PBs.

DISCUSSION

We used dengue and COVID-19 infections in adult and pediatric patients (focusing on naive B, memory B, and plasmablast cells) as a model to better understand the mechanisms that may give rise to p-PB populations in the circulation. Our results indicate that a more pro-inflammatory state in naive and memory B cells correlated with - and could influence the generation of- proliferating plasmablasts. Further exploration of these mechanisms will have implications for immune memory, vaccine development, and post-viral autoimmune syndromes.

摘要

简介

B 细胞在登革热和 COVID-19 的免疫反应中起着不可或缺的作用。先前对 COVID-19 外周浆母细胞的 scRNAseq 分析显示,存在具有不同增殖相关细胞亚群的异质群体;先前对登革热患者的研究同样表明,循环中存在增殖前浆母细胞。这些发现可能对疾病严重程度有影响。在这项研究中,我们试图深入了解与循环中增殖浆母细胞群体扩张相关的、并可能导致其扩张的幼稚 B 细胞和记忆 B 细胞中的细胞内过程。

方法

我们分析了先前发表的研究中,感染登革热(初次或二次感染)或 COVID-19(非重症或重症)的年龄匹配(儿科和成人)外周血单核细胞 scRNAseq 数据集。我们的初步分析表明,患有登革热的儿科患者和患有 COVID-19 的成年患者循环中有扩增的增殖浆母细胞(p-PB)群体。相比之下,我们的数据集中,患有登革热的成年患者和患有 COVID-19 的儿童均没有 p-PB。我们使用这一独特的初步特征来指导我们的分析设计,并将分析扩展到幼稚 B 细胞和记忆 B 细胞。

结果

在存在或不存在 p-PB 的年龄/疾病条件下,我们发现了细胞感应和激活的差异,包括 B 细胞受体和下游信号转导。同样,炎症的介导方式也不同:与没有 p-PB 的组相比,有 p-PB 的组中干扰素反应和 S100 基因的表达增加(尤其是重症 COVID-19)。此外,在有和没有 p-PB 的组中,激活、炎症和细胞命运决定的几个转录因子的表达也不同。

讨论

我们使用成人和儿科患者(专注于幼稚 B 细胞、记忆 B 细胞和浆母细胞)中的登革热和 COVID-19 感染作为模型,以更好地理解可能导致循环中 p-PB 群体产生的机制。我们的结果表明,幼稚 B 细胞和记忆 B 细胞中更具炎症性的状态与增殖浆母细胞的产生相关,并可能对其产生有影响。进一步探索这些机制将对免疫记忆、疫苗开发和病毒性自身免疫综合征产生影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/72d5/10450630/621e9d4a2c16/fimmu-14-1068424-g001.jpg

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