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炎症与结核病:宿主导向治疗。

Inflammation and tuberculosis: host-directed therapies.

机构信息

University College London, University College London Hospitals NHS Foundation Trust, London, UK.

出版信息

J Intern Med. 2015 Apr;277(4):373-87. doi: 10.1111/joim.12256. Epub 2014 May 19.

Abstract

Tuberculosis (TB) is an airborne infectious disease that kills almost two million individuals every year. Multidrug-resistant (MDR) TB is caused by strains of Mycobacterium tuberculosis (M. tb) resistant to isoniazid and rifampin, the backbone of first-line antitubercular treatment. MDR TB affects an estimated 500,000 new patients annually. Genetic analysis of drug-resistant MDR-TB showed that airborne transmission of undetected and untreated strains played a major role in disease outbreaks. The need for new TB vaccines and faster diagnostics, as well as the development of new drugs, has recently been highlighted. The major problem in terms of current TB research and clinical demands is the increasing number of cases of extensively drug-resistant and 'treatment-refractory' TB. An emerging scenario of adjunct host-directed therapies is intended to target pulmonary TB where inflammatory processes can be deleterious and lead to immune exhaustion. 'Target-organ-saving' strategies may be warranted to prevent damage to infected tissues and achieve focused, clinically relevant and long-lasting anti-M. tb cellular immune responses. Candidates for such interventions may be biological agents or already approved drugs that can be 're-purposed' to interfere with biologically relevant cellular checkpoints. Here, we review current concepts of inflammation in TB disease and discuss candidate pathways for host-directed therapies to achieve better clinical outcomes.

摘要

结核病(TB)是一种空气传播的传染病,每年导致近 200 万人死亡。耐多药结核病(MDR-TB)是由对异烟肼和利福平耐药的结核分枝杆菌(M. tb)菌株引起的,异烟肼和利福平是一线抗结核治疗的骨干。估计每年有 50 万新患者患有耐多药结核病。对耐药性 MDR-TB 的基因分析表明,未被发现和未经治疗的菌株通过空气传播在疾病爆发中起主要作用。最近强调了对新的结核病疫苗和更快速的诊断方法以及新药物的开发的需求。从当前结核病研究和临床需求的角度来看,主要问题是耐多药和“治疗难治性”结核病病例的数量不断增加。辅助宿主导向疗法的新兴方案旨在针对肺部结核病,其中炎症过程可能有害,并导致免疫衰竭。可能需要“保护靶器官”的策略来防止受感染组织受损,并实现集中,临床相关和持久的抗 M. tb 细胞免疫反应。这种干预的候选者可能是生物制剂或已经批准的药物,可以“重新定位”以干扰生物学相关的细胞检查点。在这里,我们回顾结核病疾病中炎症的当前概念,并讨论宿主导向疗法的候选途径,以实现更好的临床结果。

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