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首页> 外文期刊>Biological chemistry >Not to wake a sleeping giant: new insights into host-pathogen interactions identify new targets for vaccination against latent Mycobacterium tuberculosis infection
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Not to wake a sleeping giant: new insights into host-pathogen interactions identify new targets for vaccination against latent Mycobacterium tuberculosis infection

机译:不要唤醒沉睡的巨人:对宿主-病原体相互作用的新见解确定了针对潜在结核分枝杆菌感染的疫苗接种新目标

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摘要

Mycobacterium tuberculosis is one of the worlds' most successful and sophisticated pathogens. It is estimated that over 2 billion people today harbour latent M. tuberculosis infection without any clinical symptoms. As most new cases of active tuberculosis (TB) arise from this (growing) number of latently infected individuals, urgent measures to control TB reactivation are required, including post-exposure/therapeutic vaccines. The current bacille Calmette-Guerin (BCG) vaccine and all new generation TB vaccines being developed and tested are essentially designed as prophylactic vaccines. Unfortunately, these vaccines are unlikely to be effective in individuals already latently infected with M. tuberculosis. Here, we argue that detailed analysis of M. tuberculosis genes that are switched on predominantly during latent stage infection may lead to the identification of new antigenic targets for anti-TB strategies. We will describe essential host-pathogen interactions in TB with particular emphasis on TB latency and persistent infection. Subsequently, we will focus on novel groups of late-stage specific genes, encoded amongst others by the M. tuberculosis dormancy (dosR) regulon, and summarise recent studies describing human T-cell recognition of these dormancy antigens in relation to (latent) M. tuberculosis infection. We will discuss the possible relevance of these new classes of antigens for vaccine development against TB.
机译:结核分枝杆菌是世界上最成功,最复杂的病原体之一。据估计,当今有超过20亿人患有潜伏的结核分枝杆菌感染,没有任何临床症状。由于大多数活动性肺结核(TB)的新病例都源于这种(不断增长)的潜伏感染个体,因此需要采取紧急措施来控制TB的再激活,包括暴露后/治疗性疫苗。目前,正在研发和测试的杆菌卡介苗疫苗(BCG)和所有新一代结核病疫苗实质上都是作为预防性疫苗而设计的。不幸的是,这些疫苗在已经潜伏感染了结核分枝杆菌的个体中不太可能有效。在这里,我们认为详细分析主要在潜伏期感染期间打开的结核分枝杆菌基因可能会导致抗结核策略新抗原靶标的鉴定。我们将描述结核病中必不可少的宿主-病原体相互作用,并特别强调结核病潜伏期和持续感染。随后,我们将重点关注由结核分枝杆菌休眠(dosR)调控基因编码的新型晚期特定基因组,并总结了最近的研究,这些研究描述了人类T细胞识别这些与(潜伏)M有关的休眠抗原结核感染我们将讨论这些新型抗原与抗结核疫苗开发的相关性。

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