衰老相关B细胞在疾病中的功能与调控

IF 4.5 2区 生物学 Q2 CELL BIOLOGY Journal of Cellular Physiology Pub Date : 2025-01-03 DOI:10.1002/jcp.31522
Zi Geng, Yejin Cao, Longhao Zhao, Likun Wang, Yingjie Dong, Yujing Bi, Guangwei Liu
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引用次数: 0

摘要

衰老过程经常导致免疫相关疾病,包括感染、肿瘤和自身免疫性疾病。最近,研究人员在老年雌性小鼠中发现了一个特殊的B细胞亚群,该亚群随着年龄的增长而增加,并在自身免疫性疾病或病毒感染的小鼠模型中过早积累;这些B细胞被称为年龄相关B细胞(abc)。这些细胞具有独特的细胞表面表型和转录特征,细胞群被广泛认为是CD11c+CD11b+T-bet+CD21-CD23-细胞。研究表明,abc是一种异质的B细胞群,它们独立于生发中心产生,对B细胞受体(BCR)和CD40刺激不敏感,在toll样受体7 (TLR7)和IL-21刺激下分化和增殖。此外,它们分泌自身抗体和细胞因子来调节免疫反应。这些问题引起了该领域研究者的广泛关注。本文综述了近年来有关抗体的研究进展,包括抗体在衰老、病毒感染、自身免疫性疾病、器官移植等方面的功能和调控。
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Function and Regulation of Age-Associated B Cells in Diseases

The aging process often leads to immune-related diseases, including infections, tumors, and autoimmune disorders. Recently, researchers identified a special subpopulation of B cells in elderly female mice that increases with age and accumulates prematurely in mouse models of autoimmune diseases or viral infections; these B cells are known as age-related B cells (ABCs). These cells possess distinctive cell surface phenotypes and transcriptional characteristics, and the cell population is widely recognized as CD11c+CD11b+T-bet+CD21-CD23- cells. Research has shown that ABCs are a heterogeneous group of B cells that originate independently of the germinal center and are insensitive to B-cell receptor (BCR) and CD40 stimulation, differentiating and proliferating in response to toll-like receptor 7 (TLR7) and IL-21 stimulation. Additionally, they secrete self-antibodies and cytokines to regulate the immune response. These issues have aroused widespread interest among researchers in this field. This review summarizes recent research progress on ABCs, including the functions and regulation of ABCs in aging, viral infection, autoimmune diseases, and organ transplantation.

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来源期刊
CiteScore
14.70
自引率
0.00%
发文量
256
审稿时长
1 months
期刊介绍: The Journal of Cellular Physiology publishes reports of high biological significance in areas of eukaryotic cell biology and physiology, focusing on those articles that adopt a molecular mechanistic approach to investigate cell structure and function. There is appreciation for the application of cellular, biochemical, molecular and in vivo genetic approaches, as well as the power of genomics, proteomics, bioinformatics and systems biology. In particular, the Journal encourages submission of high-interest papers investigating the genetic and epigenetic regulation of proliferation and phenotype as well as cell fate and lineage commitment by growth factors, cytokines and their cognate receptors and signal transduction pathways that influence the expression, integration and activities of these physiological mediators. Similarly, the Journal encourages submission of manuscripts exploring the regulation of growth and differentiation by cell adhesion molecules in addition to the interplay between these processes and those induced by growth factors and cytokines. Studies on the genes and processes that regulate cell cycle progression and phase transition in eukaryotic cells, and the mechanisms that determine whether cells enter quiescence, proliferate or undergo apoptosis are also welcomed. Submission of papers that address contributions of the extracellular matrix to cellular phenotypes and physiological control as well as regulatory mechanisms governing fertilization, embryogenesis, gametogenesis, cell fate, lineage commitment, differentiation, development and dynamic parameters of cell motility are encouraged. Finally, the investigation of stem cells and changes that differentiate cancer cells from normal cells including studies on the properties and functions of oncogenes and tumor suppressor genes will remain as one of the major interests of the Journal.
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