Activation dynamics of antigen presenting cells in vivo against Mycobacterium bovis BCG in different immunized route.

IF 2.9 4区 医学 Q3 IMMUNOLOGY BMC Immunology Pub Date : 2023-11-27 DOI:10.1186/s12865-023-00589-6
Zhengzhong Xu, Xin Li, Aihong Xia, Zhifang Zhang, Jiaxu Wan, Yan Gao, Chuang Meng, Xiang Chen, Xin-An Jiao
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Abstract

Background: Control of Tuberculosis (TB) infection is mainly the result of productive teamwork between T-cell populations and antigen presenting cells (APCs). However, APCs activation at the site of initiating cellular immune response during BCG early infection is not completely understood.

Methods: In this study, we injected C57BL/6 mice in intravenous (i.v) or subcutaneous (s.c) route, then splenic or inguinal lymph node (LN) DCs and MΦs were sorted, and mycobacteria uptake, cytokine production, antigen presentation activity, and cell phenotype were investigated and compared, respectively.

Results: Ag85A-specific T-cell immune response began at 6 days post BCG infection, when BCG was delivered in s.c route, Th17 immune response could be induced in inguinal LN. BCG could induce high level of activation phenotype in inguinal LN MΦs, while the MHC II presentation of mycobacteria-derived peptides by DCs was more efficient than MΦs.

Conclusions: The results showed that BCG immunized route can decide the main tissue of T-cell immune response. Compared with s.c injected route, APCs undergo more rapid cell activation in spleen post BCG i.v infection.

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不同免疫途径下抗原提呈细胞体内对牛分枝杆菌卡介苗的活化动力学。
背景:结核病(TB)感染的控制主要是t细胞群和抗原呈递细胞(APCs)高效合作的结果。然而,在卡介苗早期感染过程中,APCs在细胞免疫应答起始部位的激活尚不完全清楚。方法:采用静脉(i.v)或皮下(s.c)给小鼠注射C57BL/6,分别对小鼠脾或腹股沟淋巴结(LN) DCs和MΦs进行分选,观察并比较分枝杆菌摄取、细胞因子产生、抗原呈递活性和细胞表型。结果:卡介苗感染后6天开始出现ag85a特异性t细胞免疫应答,当卡介苗经s.c途径给药时,可在腹股沟LN中诱导Th17免疫应答。卡介苗在腹股沟LN中可诱导高水平的活化表型MΦs,而dc对分枝杆菌衍生肽的MHC II呈递比MΦs更有效。结论:卡介苗免疫途径可决定t细胞免疫应答的主要组织。卡介苗感染后,APCs在脾脏的细胞活化速度比s.c注射更快。
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来源期刊
BMC Immunology
BMC Immunology 医学-免疫学
CiteScore
5.50
自引率
0.00%
发文量
54
审稿时长
1 months
期刊介绍: BMC Immunology is an open access journal publishing original peer-reviewed research articles in molecular, cellular, tissue-level, organismal, functional, and developmental aspects of the immune system as well as clinical studies and animal models of human diseases.
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