腺样体扁桃体肥大相关B细胞免疫活化调控机制的研究进展  

作　　者：陈雯婧[1] 高瑞雨 黄婧雯 叶京英[1] 刘万里[2] Chen Wenjing;Gao Ruiyu;Huang Jingwen;Ye Jingying;Liu Wanli(Department of Otolaryngology-Head and Neck Surgery,Beijing Tsinghua Changgung Hospital,School of Clinical Medicine,Institute for Precision Medicine,Tsinghua University,Beijing 102218,China;School of Life Sciences,Institute for Immunology,Tsinghua University,Tsinghua-Peking Center for Life Sciences,State Key Laboratory of Membrane Biology,Ministry of Education Key Laboratory of Protein Sciences,Beijing Key Lab for Immunological Research on Chronic Diseases,Beijing 100084,China)

机构地区：[1]清华大学附属北京清华长庚医院耳鼻喉头颈外科,清华大学临床医学院,清华大学精准医学研究院,北京102218 [2]清华大学生命科学学院免疫研究所,清华北大生命科学联合中心,膜生物学全国重点实验室,蛋白质科学教育部重点实验室,北京市慢性病的免疫学研究重点实验室,北京100084

出　　处：《生物医学转化》2024年第2期81-90,共10页Biomedical transformation

基　　金：国家重点研发计划项目(2021YFC2300500,2021YFC2302403);国家自然科学基金项目(32141004,81825010,82371132,82341247);北京市自然科学基金项目(23Z30090);北京市属医院科研培育计划项目(PX2022040)。

摘　　要：B细胞通过其表面分布的B细胞受体(BCR)识别外界抗原,是机体产生保护性抗体与免疫记忆的关键步骤。B细胞免疫活化调控与诸多上呼吸道疾病是密切相关的。儿童常见疾病腺样体扁桃体肥大(ATH),其特征性病理本质为淋巴滤泡的增生,但其确切机制尚未明确。本文综述静息态下维持B细胞存活的BCR滋养信号研究,阐述了B细胞免疫活化及产生快速高效免疫记忆的调控机制,尤其是活化早期分子事件,强调mIgG-tail对记忆性抗体应答的相关作用。B细胞活化调控过程出现异常可破坏免疫稳态平衡,导致疾病的发生。本文总结了B细胞免疫活化调控与ATH的机制关联,尝试探讨信号转导通路失调或突变对ATH的可能影响。旨在深入理解ATH的致病机理,以期挖掘潜在研究突破口,寻找ATH新的诊疗靶点。B cells play a crucial role in recognizing external antigens through their surface B cell receptor(BCR),essential for generating protective antibodies and immune memory.Regulation of B cell immune activation is closely linked to various upper respiratory tract diseases.Adenoid hypertrophy(ATH),a common childhood condition,is characterized by lymphoid follicular hyperplasia,yet its exact mechanisms remain elusive.This review consolidates research on BCR trophic signaling that sustains B cell viability in resting state.It clarifies the regulatory mechanisms governing B cell immune activation and the establishment of rapid,effective immune memory,with a specific focus on early molecular activation events and the pivotal role of mIgG-tail in memory antibody responses.Dysregulation of B cell activation processes can disrupt immune balance,potentially precipitating disease.This synthesis explores the connection between regulation of B cell activation and ATH pathogenesis,examining the potential impacts of signaling pathway dysregulation or mutations on ATH.The review aims to enhance understanding of the disease mechanisms underlying ATH,with the goal of identifying new diagnostic and therapeutic targets for this condition.

关 键 词：腺样体扁桃体肥大 B细胞 B细胞活化 B细胞受体 免疫突触 

分 类 号：R766[医药卫生—耳鼻咽喉科] R392[医药卫生—临床医学]