Establishment of CD1b-restricted immunity to lipid antigens in the pulmonary response to Mycobacterium tuberculosis infection.

IF 2.9 3区 医学 Q3 IMMUNOLOGY
Macallister C Harris, Hadley E Gary, Sarah K Cooper, David F Ackart, James E DiLisio, Randall J Basaraba, Tan-Yun Cheng, Ildiko van Rhijn, D Branch Moody, Brendan K Podell
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Abstract

CD1 is an antigen-presenting glycoprotein homologous to MHC I; however, CD1 proteins present lipid rather than peptide antigens. CD1 proteins are well established to present lipid antigens of Mycobacterium tuberculosis (Mtb) to T cells, but understanding the role of CD1-restricted immunity in vivo in response to Mtb infection has been limited by the availability of animal models naturally expressing the CD1 proteins implicated in human response: CD1a, CD1b, and CD1c. Guinea pigs, in contrast to other rodent models, express four CD1b orthologs, and here we utilize the guinea pig to establish the kinetics of gene and protein expression of CD1b orthologs, as well as the Mtb lipid-antigen and CD1b-restricted immune response at the tissue level over the course of Mtb infection. Our results indicate transient upregulation of CD1b expression during the effector phase of adaptive immunity that wanes with disease chronicity. Gene expression indicates that the upregulation of CD1b is the result of transcriptional induction across all CD1b orthologs. We show high CD1b3 expression on B cells, and identify CD1b3 as the predominant CD1b ortholog in pulmonary granuloma lesions. We identify ex vivo cytotoxic activity directed against CD1b that parallels the kinetic changes in CD1b expression in Mtb-infected lungs and spleen. This study confirms that CD1b expression is modulated by Mtb infection in lung and spleen, leading to pulmonary and extrapulmonary CD1b-restricted immunity as a component of the antigen-specific response to Mtb infection.

在肺部对结核分枝杆菌感染的反应中建立对脂质抗原的 CD1b 限制性免疫。
CD1 是一种抗原递呈糖蛋白,与 MHC I 同源;但 CD1 蛋白递呈的是脂质抗原而不是肽抗原。CD1 蛋白能向 T 细胞呈递结核分枝杆菌(Mtb)的脂质抗原,这一点已得到证实,但由于缺乏天然表达与人类反应有关的 CD1 蛋白的动物模型,人们对 CD1 限制性免疫在体内应对 Mtb 感染的作用的了解一直受到限制:CD1a、CD1b 和 CD1c。与其他啮齿类动物模型不同,豚鼠能表达四种 CD1b 同源物。在此,我们利用豚鼠建立了 CD1b 同源物的基因和蛋白表达动力学,以及在 Mtb 感染过程中组织水平上的 Mtb 脂质抗原和 CD1b 限制性免疫反应。我们的研究结果表明,在适应性免疫的效应阶段,CD1b的表达有短暂的上调,这种上调会随着疾病的慢性化而减弱。基因表达表明,CD1b 的上调是所有 CD1b 同源物转录诱导的结果。我们发现 CD1b3 在 B 细胞上高表达,并确定 CD1b3 是肺肉芽肿病变中最主要的 CD1b 同源物。我们发现针对 CD1b 的体外细胞毒性活性与受 Mtb 感染的肺部和脾脏中 CD1b 表达的动力学变化相似。这项研究证实,CD1b的表达受肺部和脾脏Mtb感染的调节,导致肺部和肺外CD1b限制性免疫,成为Mtb感染抗原特异性反应的一个组成部分。
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来源期刊
Infection and Immunity
Infection and Immunity 医学-传染病学
CiteScore
6.00
自引率
6.50%
发文量
268
审稿时长
3 months
期刊介绍: Infection and Immunity (IAI) provides new insights into the interactions between bacterial, fungal and parasitic pathogens and their hosts. Specific areas of interest include mechanisms of molecular pathogenesis, virulence factors, cellular microbiology, experimental models of infection, host resistance or susceptibility, and the generation of innate and adaptive immune responses. IAI also welcomes studies of the microbiome relating to host-pathogen interactions.
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