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IgD 年龄相关 B 细胞是感染后主要 T 细胞非依赖 B 细胞反应的祖细胞,该反应产生保护性抗体,并可被衰老个体中的灭活疫苗诱导。

IgD age-associated B cells are the progenitors of the main T-independent B cell response to infection that generates protective Ab and can be induced by an inactivated vaccine in the aged.

机构信息

Department of Pathology, University of Massachusetts Chan Medical School, Worcester, Massachusetts, USA.

College of Veterinary Medicine, North Carolina State University, Raleigh, North Carolina, USA.

出版信息

Aging Cell. 2022 Oct;21(10):e13705. doi: 10.1111/acel.13705. Epub 2022 Sep 2.

Abstract

Age-associated B cells (ABC) accumulate with age and are associated with autoimmunity and chronic infection. However, their contributions to acute infection in the aged and their developmental pathways are unclear. We find that the response against influenza A virus infection in aged mice is dominated by a Fas GL7 effector B cell population we call infection-induced ABC (iABC). Most iABC express IgM and include antibody-secreting cells in the spleen, lung, and bone marrow. We find that in response to influenza, IgD CD21 CD23 ABC are the precursors of iABC and become memory B cells. These IgD ABC develop in germ-free mice, so are independent of foreign antigen recognition. The response of ABC to influenza infection, resulting in iABC, is T cell independent and requires both extrinsic TLR7 and TLR9 signals. In response to influenza infection, IgD ABC can induce a faster recovery of weight and higher total anti-influenza IgG and IgM titers that can neutralize virus. Immunization with whole inactivated virus also generates iABC in aged mice. Thus, in unimmunized aged mice, whose other B and T cell responses have waned, IgD ABC are likely the naive B cells with the potential to become Ab-secreting cells and to provide protection from infection in the aged.

摘要

与年龄相关的 B 细胞(ABC)随年龄增长而积累,与自身免疫和慢性感染有关。然而,它们对老年急性感染的贡献及其发育途径尚不清楚。我们发现,老年小鼠对甲型流感病毒感染的反应主要由 Fas GL7 效应 B 细胞群体主导,我们称之为感染诱导的 ABC(iABC)。大多数 iABC 表达 IgM,并包括脾脏、肺和骨髓中的抗体分泌细胞。我们发现,针对流感,IgD CD21 CD23 ABC 是 iABC 的前体,并成为记忆 B 细胞。这些 IgD ABC 在无菌小鼠中发育,因此不依赖于外来抗原识别。ABC 对流感感染的反应导致 iABC 的产生是 T 细胞非依赖性的,需要外在的 TLR7 和 TLR9 信号。针对流感感染,IgD ABC 可以诱导体重更快恢复,以及更高的总抗流感 IgG 和 IgM 滴度,从而中和病毒。用全灭活病毒免疫也会在老年小鼠中产生 iABC。因此,在未免疫的老年小鼠中,其其他 B 和 T 细胞反应已经减弱,IgD ABC 可能是具有成为抗体分泌细胞并为老年提供感染保护潜力的幼稚 B 细胞。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d20f/9577953/1d76e3d34c30/ACEL-21-e13705-g003.jpg

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