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在卡介苗接种地区对麻风病和结核病患者针对麻风分枝杆菌和结核分枝杆菌GroES的15肽进行免疫分析:对疫苗和诊断试剂开发的启示

Immune profiling of leprosy and tuberculosis patients to 15-mer peptides of Mycobacterium leprae and M. tuberculosis GroES in a BCG vaccinated area: implications for development of vaccine and diagnostic reagents.

作者信息

Hussain Rabia, Shahid Firdaus, Zafar Shahid, Dojki Maqboola, Dockrell Hazel M

机构信息

Department of Pathology and Microbiology, Aga Khan University, PO Box 3500, Karachi, Pakistan.

出版信息

Immunology. 2004 Apr;111(4):462-71. doi: 10.1111/j.0019-2805.2004.01839.x.

Abstract

Mycobacterium leprae (ML) GroES has been shown to induce strong T cell responses in tuberculoid as well as in exposed healthy contacts of leprosy patients, and therefore this antigen has been the focus of study as a potential vaccine candidate. Paradoxically, we have shown that ML GroES also induces extremely high titres of IgG1 antibody in leprosy patients across the disease spectrum, a response associated with disease progression. IgG1 antibodies in leprosy also show a negative association with interferon-gamma, a critical T cell cytokine responsible for macrophage activation and intracellular killing of mycobacteria. We therefore queried if antibody and T cell responses were being evoked by different epitopes in ML GroES proteins. To address the issue of epitope recognition in mycobacterial diseases, we have analysed 16 peptides (15-mer peptides) spanning the entire ML and M. tuberculosis GroES protein in leprosy (n = 19) and tuberculosis (n = 9) patients and healthy endemic controls (n = 8). Our analysis demonstrates clearly that the dominant peptides evokingT cell and IgG subclass antibodies were different. The target of both T and B cell responses were cross-reactive epitopes in all groups. Differences in disease and healthy states related to the strength (mean intensity) of the T cell and antibody response. IgG1 and IgG3 antibodies were associated with disseminated disease and IgG 2 and IgG4 with disease limitation. Such comprehensive immune profiling of antigen-specific responses is critical to understanding the disease pathogenesis and also if these reagents are to be exploited for either diagnostic or vaccine purposes.

摘要

麻风分枝杆菌(ML)热休克蛋白10(GroES)已被证明在结核样型麻风患者以及麻风患者的接触者中可诱导强烈的T细胞反应,因此,该抗原作为一种潜在的疫苗候选物一直是研究的重点。矛盾的是,我们发现ML GroES在整个疾病谱的麻风患者中也可诱导产生极高滴度的IgG1抗体,这种反应与疾病进展相关。麻风患者体内的IgG1抗体还与γ干扰素呈负相关,γ干扰素是一种关键的T细胞细胞因子,负责巨噬细胞活化和对分枝杆菌的细胞内杀伤。因此,我们推测ML GroES蛋白中不同的表位是否会引发抗体和T细胞反应。为了解决分枝杆菌疾病中表位识别的问题,我们分析了16种肽段(15聚体肽段),这些肽段覆盖了麻风患者(n = 19)、肺结核患者(n = 9)和健康地方病对照者(n = 8)体内完整的ML和结核分枝杆菌GroES蛋白。我们的分析清楚地表明,引发T细胞和IgG亚类抗体的主要肽段是不同的。所有组中T细胞和B细胞反应的靶点都是交叉反应性表位。疾病状态和健康状态的差异与T细胞和抗体反应的强度(平均强度)有关。IgG1和IgG3抗体与播散性疾病相关,而IgG2和IgG4与疾病局限相关。这种对抗原特异性反应的全面免疫分析对于理解疾病发病机制以及这些试剂是否用于诊断或疫苗目的至关重要。

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