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潜伏性结核感染的动态再感染假说。

A dynamic reinfection hypothesis of latent tuberculosis infection.

作者信息

Cardona P-J

机构信息

Dept. of Microbiology, Germans Trias I Pujol Health Science Research Institute Foundation, Autonomous University of Barcelona, Badalona, Catalonia, Spain.

出版信息

Infection. 2009 Apr;37(2):80-6. doi: 10.1007/s15010-008-8087-y. Epub 2009 Mar 23.

Abstract

BACKGROUND

It has been traditionally postulated that individuals, once infected by Mycobacterium tuberculosis, will retain throughout their entire lifetime latent bacilli which will remain dormant in old lesions. This bacillus would then be the source of a later reactivation of active tuberculosis (TB), with the aid of resuscitation factors. Unfortunately, the presence of these bacilli can only be predicted by indirect immunological methods, such as the tuberculin skin test (TST) or T cell interferon-gamma release assays. Other evidence shows that a 9-month isoniazid treatment of TST+ individuals converting to TB reduces the incidence of TB by approximately 90%.

QUESTIONS

Taking into account this widely accepted framework, I suggest that there are at least three relevant questions to answer: (1) How can dormant bacilli remain in the lungs for an entire lifetime, taking into account constant cellular turnover and the healing of damaged tissues? (2) What provides the resuscitation factor to dormant bacilli, assuming that these latent bacilli are indeed present inside old lesions? (3) Why can a 9-month treatment with isoniazid eliminate dormant bacilli? As isoniazid is active only against growing bacilli, and thus is only able to destroy them after reactivation of latent bacilli, this treatment should have to be provided for life if the traditionally accepted postulate is correct.

HYPOTHESIS

For a better understanding of latent TB infection. I propose a hypothesis that describes a dynamic scenario of constant endogenous reinfection with M. tuberculosis which explains the efficacy of the current standard of treatment. If this hypothesis is true, new strategies for the management of TB may arise.

摘要

背景

传统观点认为,个体一旦感染结核分枝杆菌,一生中都会携带潜伏性杆菌,这些杆菌会在陈旧病灶中保持休眠状态。在复苏因子的作用下,这些杆菌将成为日后活动性结核病重新激活的源头。不幸的是,这些杆菌的存在只能通过间接免疫方法预测,如结核菌素皮肤试验(TST)或T细胞干扰素-γ释放检测。其他证据表明,对结核菌素试验阳性且已转化为结核病的个体进行9个月的异烟肼治疗可使结核病发病率降低约90%。

问题

考虑到这一被广泛接受的框架,我认为至少有三个相关问题需要回答:(1)考虑到细胞的持续更新和受损组织的愈合,休眠杆菌如何能在肺部留存一生?(2)假设这些潜伏性杆菌确实存在于陈旧病灶中,是什么为休眠杆菌提供了复苏因子?(3)为什么异烟肼9个月的治疗就能消除休眠杆菌?由于异烟肼仅对生长中的杆菌有活性,因此只有在潜伏性杆菌重新激活后才能将其消灭,如果传统观点正确,这种治疗应该持续终身。

假设

为了更好地理解潜伏性结核感染。我提出一个假设,该假设描述了结核分枝杆菌持续内源性再感染的动态情况,解释了当前标准治疗的疗效。如果这个假设是正确的,可能会产生新的结核病管理策略。

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