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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >T Cell Immunity to the Alkyl Hydroperoxide Reductase of Burkholderia pseudomallei: A Correlate of Disease Outcome in Acute Melioidosis
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T Cell Immunity to the Alkyl Hydroperoxide Reductase of Burkholderia pseudomallei: A Correlate of Disease Outcome in Acute Melioidosis

机译:T细胞免疫的伯克霍尔德菌假mallei的烷基氢过氧化物还原酶:急性类痔病的疾病结果的相关性。

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摘要

There is an urgent need for a better understanding of adaptive immunity to Burkholderia pseudomallei, the causative agent of melioidosis that is frequently associated with sepsis or death in patients in Southeast Asia and Northern Australia. The imperative to identify vaccine targets is driven both by the public health agenda in these regions and biological threat concerns. In several intracellular bacterial pathogens, alkyl hydroperoxidase reductases are upregulated as part of the response to host oxidative stress, and they can stimulate strong adaptive immunity. We show that alkyl hydroperoxidase reductase (AhpC) of B. pseudomallei is strongly immunogenic for T cells of 'humanized' HLA transgenic mice and seropositive human donors. Some T cell epitopes, such as p6, are able to bind diverse HLA class II heterodimers and stimulate strong T cell immunity in mice and humans. Importantly, patients with acute melioidosis who survive infection show stronger T cell responses to AhpC relative to those who do not. Although the sequence of AhpC is virtually invariant among global B. pseudomallei clinical isolates, a Cambodian isolate varies only in C-terminal truncation of the p6 T cell epitope, raising the possibility of selection by host immunity. This variant peptide is virtually unable to stimulate T cell immunity. For an infection in which there has been debate about centrality of T cell immunity in defense, these observations support a role for T cell immunity to AhpC in disease protection.
机译:迫切需要更好地理解针对假鼻疽伯克霍尔德氏菌的适应性免疫,该病是类鼻疽的病原体,经常与东南亚和北澳大利亚患者的败血症或死亡相关。这些地区的公共卫生议程和对生物威胁的关注都决定了疫苗目标的迫切性。在几种细胞内细菌病原体中,烷基氢过氧化物酶还原酶被上调,作为对宿主氧化应激反应的一部分,它们可以刺激强大的适应性免疫。我们表明,烷基氢过氧化物酶还原酶(AhpC)的假苹果芽孢杆菌对“人源化” HLA转基因小鼠和血清反应阳性人类供体的T细胞具有强免疫原性。一些T细胞表位(例如p6)能够结合多种HLA II类异二聚体,并在小鼠和人类中刺激强大的T细胞免疫力。重要的是,与未感染者相比,幸存下来的患有急性类鼻疽病的患者对AhpC的T细胞反应更强。尽管AhpC的序列实际上在全球假性疟原虫临床分离株中是不变的,但柬埔寨分离株仅在p6 T细胞表位的C端截短方面有所不同,从而增加了通过宿主免疫进行选择的可能性。该变体肽实际上不能刺激T细胞免疫。对于关于T细胞免疫在防御中的中心地位存在争议的感染,这些观察结果支持T细胞针对AhpC的免疫对疾病保护的作用。

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