Department of Medicine, University of Washington School of Medicine, Seattle, Washington, United States of America.
PLoS Pathog. 2011 Aug;7(8):e1002174. doi: 10.1371/journal.ppat.1002174. Epub 2011 Aug 11.
The development of effective immunoprophylaxis against tuberculosis (TB) remains a global priority, but is hampered by a partially protective Bacillus Calmette-Guérin (BCG) vaccine and an incomplete understanding of the mechanisms of immunity to Mycobacterium tuberculosis. Although host genetic factors may be a primary reason for BCG's variable and inadequate efficacy, this possibility has not been intensively examined. We hypothesized that Toll-like receptor (TLR) variation is associated with altered in vivo immune responses to BCG. We examined whether functionally defined TLR pathway polymorphisms were associated with T cell cytokine responses in whole blood stimulated ex vivo with BCG 10 weeks after newborn BCG vaccination of South African infants. In the primary analysis, polymorphism TLR6_C745T (P249S) was associated with increased BCG-induced IFN-γ in both discovery (n = 240) and validation (n = 240) cohorts. In secondary analyses of the combined cohort, TLR1_T1805G (I602S) and TLR6_G1083C (synonymous) were associated with increased IFN-γ, TLR6_G1083C and TLR6_C745T were associated with increased IL-2, and TLR1_A1188T was associated with increased IFN-γ and IL-2. For each of these polymorphisms, the hypo-responsive allele, as defined by innate immunity signaling assays, was associated with increased production of TH1-type T cell cytokines (IFN-γ or IL-2). After stimulation with TLR1/6 lipopeptide ligands, PBMCs from TLR1/6-deficient individuals (stratified by TLR1_T1805G and TLR6_C745T hyporesponsive genotypes) secreted lower amounts of IL-6 and IL-10 compared to those with responsive TLR1/6 genotypes. In contrast, no IL-12p70 was secreted by PBMCs or monocytes. These data support a mechanism where TLR1/6 polymorphisms modulate TH1 T-cell polarization through genetic regulation of monocyte IL-10 secretion in the absence of IL-12. These studies provide evidence that functionally defined innate immune gene variants are associated with the development of adaptive immune responses after in vivo vaccination against a bacterial pathogen in humans. These findings could potentially guide novel adjuvant vaccine strategies as well as have implications for IFN-γ-based diagnostic testing for TB.
针对结核病(TB)的有效免疫预防仍然是全球重点,但由于卡介苗(BCG)疫苗部分保护作用以及对结核分枝杆菌免疫机制的不完全了解而受到阻碍。尽管宿主遗传因素可能是 BCG 疗效差异和不充分的主要原因,但这一可能性尚未得到深入研究。我们假设 Toll 样受体(TLR)的变异与 BCG 体内免疫反应的改变有关。我们研究了功能定义的 TLR 通路多态性是否与南非婴儿接种 BCG 后 10 周全血刺激体外 BCG 诱导的 T 细胞细胞因子反应有关。在初步分析中,TLR6_C745T(P249S)多态性与发现队列(n=240)和验证队列(n=240)中 BCG 诱导的 IFN-γ增加有关。在合并队列的二次分析中,TLR1_T1805G(I602S)和 TLR6_G1083C(同义)与 IFN-γ增加有关,TLR6_G1083C 和 TLR6_C745T 与 IL-2 增加有关,TLR1_A1188T 与 IFN-γ和 IL-2 增加有关。对于这些多态性中的每一个,在先天免疫信号测定中定义的低反应等位基因与 TH1 型 T 细胞细胞因子(IFN-γ或 IL-2)的产生增加有关。用 TLR1/6 脂肽配体刺激后,TLR1/6 缺陷个体的 PBMC(根据 TLR1_T1805G 和 TLR6_C745T 低反应基因型分层)分泌的 IL-6 和 IL-10 量低于具有反应性 TLR1/6 基因型的个体。相比之下,PBMC 或单核细胞不分泌 IL-12p70。这些数据支持这样一种机制,即 TLR1/6 多态性通过遗传调节单核细胞 IL-10 分泌来调节 TH1 T 细胞极化,而不分泌 IL-12。这些研究提供了证据,证明功能定义的先天免疫基因变异与人类针对细菌病原体进行体内疫苗接种后适应性免疫反应的发展有关。这些发现可能为新型佐剂疫苗策略提供指导,并对基于 IFN-γ的结核病诊断测试产生影响。
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