Understanding the Heterogeneous Population of Age-Associated B Cells and Their Contributions to Autoimmunity and Immune Response to Pathogens

Overview

Journal Crit Rev Immunol

Publisher Begell House

Specialty Allergy & Immunology

Date 2021 Jan 11

PMID 33426819

Citations 4

Authors

Olivia Kugler-Umana

Priyadharshini Devarajan

Susan L Swain

Affiliations

Soon will be listed here.

Abstract

In humans and mice, susceptibility to infections and autoimmunity increases with age due to age-associated changes in innate and adaptive immune responses. Aged innate cells are also less active, leading to decreased naive T- and B-cell responses. Aging innate cells contribute to an overall heightened inflammatory environment. Naive T and B cells undergo cell-intrinsic age-related changes that result in reduced effector and memory responses. However, previously established B- and T-cell memory responses persist with age. One dramatic change is the appearance of a newly recognized population of age-associated B cells (ABCs) that has a unique cluster of differentiation (CD)21-CD23- phenotype. Here, we discuss the discovery and origins of the naive phenotype immunoglobulin (Ig)D+ versus activated CD11c+T-bet+ ABCs, with a focus on protective and pathogenic properties. In humans and mice, antigen-experienced CD11c+T-bet+ ABCs increase with autoimmunity and appear in response to bacterial and viral infections. However, our analyses indicate that CD21-CD23- ABCs include a resting, naive, progenitor ABC population that expresses IgD. Similar to generation of CD11c+T-bet+ ABCs, naive ABC response to pathogens depends on toll-like receptor stimulation, making this a key feature of ABC activation. Here, we put forward a potential developmental map of distinct subsets from putative naive ABCs. We suggest that defining signals that can harness the naive ABC response may contribute to protection against pathogens in the elderly. CD11c+T-bet+ ABCs may be useful targets for therapeutic strategies to counter autoimmunity.

Citing Articles

Increased development of T-betCD11c B cells predisposes to lupus in females: Analysis in BXD2 mouse and genetic crosses.

Sullivan K, Chapman C, Lu L, Ashbrook D, Wang Y, Alduraibi F Clin Immunol. 2023; 257:109842.

PMID: 37981105 PMC: 10799694. DOI: 10.1016/j.clim.2023.109842.

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.

Kugler-Umana O, Zhang W, Kuang Y, Liang J, Castonguay C, Tonkonogy S Aging Cell. 2022; 21(10):e13705.

PMID: 36056604 PMC: 9577953. DOI: 10.1111/acel.13705.

"An Intrinsic Program Determines Key Age-Associated Changes in Adaptive Immunity that Limit Response to Non-Pathogens.".

Swain S, Kugler-Umana O, Tonkonogy S Front Aging. 2022; 2.

PMID: 35382063 PMC: 8979546. DOI: 10.3389/fragi.2021.701900.

Finger C, Moreno-Gonzalez I, Gutierrez A, Moruno-Manchon J, McCullough L Mol Psychiatry. 2021; 27(2):803-818.

PMID: 34711943 PMC: 9046462. DOI: 10.1038/s41380-021-01361-1.

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