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成人结核性脑膜炎及其并发症的治疗

Treatment of Tuberculous Meningitis and Its Complications in Adults.

作者信息

Davis Angharad, Meintjes Graeme, Wilkinson Robert J

机构信息

National Hospital for Neurology and Neurosurgery, University College London Hospitals, London, WC1N 3BG, UK.

University College London, Gower Street, London, WC1E 6BT, UK.

出版信息

Curr Treat Options Neurol. 2018 Feb 28;20(3):5. doi: 10.1007/s11940-018-0490-9.

Abstract

PURPOSE OF REVIEW

Tuberculous meningitis (TBM) is a global health problem. In this review, we systematically evaluate the evidence for current and emerging antimicrobials, host-directed therapies and supportive managements.

RECENT FINDINGS

Current antimicrobial regimes do not factor the differing ability of drugs to cross the blood-brain barrier. Rifampicin may be more effective at higher doses yet the most recent clinical trial failed to demonstrate survival benefit at 15 mg/kg/day. Dose finding studies suggest that higher doses still may be safe and more effective. Fluoroquinolones are currently listed as important second-line agents in drug-resistant TBM; however, a survival benefit as a first-line agent has yet to be shown. Linezolid may be a promising antimicrobial with good central nervous system penetrance. Dexamethasone reduces mortality in HIV-uninfected individuals yet evidence for its use in HIV co-infection is lacking. Aspirin has anti-inflammatory and anti-thrombotic properties. Small studies have demonstrated efficacy in reducing stroke but further research is required to better understand its effect on controlling the host inflammatory response. Discovery of genetic polymorphisms may direct individualized immune therapies and mediators of the innate immune response may provide targets for the development of novel therapies. There is at present no significant evidence base to guide management of hydrocephalus in HIV co-infection. Further clinical trial data is required to improve treatment outcomes in TBM in particularly in regard to the value of high-dose rifampicin, newer antimicrobials with improved central nervous system penetration and host-directed therapies. Supportive measures in particular the management of hydrocephalus in HIV co-infection should be an area for future research.

摘要

综述目的

结核性脑膜炎(TBM)是一个全球性的健康问题。在本综述中,我们系统地评估了当前及新出现的抗微生物药物、宿主导向疗法和支持性治疗的证据。

最新发现

当前的抗微生物治疗方案未考虑药物穿越血脑屏障能力的差异。利福平在较高剂量时可能更有效,但最近的临床试验未能证明15mg/kg/天的剂量能带来生存获益。剂量探索研究表明,更高剂量可能仍然安全且更有效。氟喹诺酮类药物目前被列为耐药性TBM的重要二线药物;然而,作为一线药物的生存获益尚未得到证实。利奈唑胺可能是一种有前景的抗微生物药物,具有良好的中枢神经系统穿透力。地塞米松可降低未感染HIV个体的死亡率,但缺乏其用于合并HIV感染患者的证据。阿司匹林具有抗炎和抗血栓特性。小型研究已证明其在减少中风方面的疗效,但需要进一步研究以更好地了解其对控制宿主炎症反应的作用。基因多态性的发现可能指导个体化免疫治疗,先天免疫反应的介质可能为新型疗法的开发提供靶点。目前尚无重要的证据基础来指导合并HIV感染时脑积水的管理。需要更多的临床试验数据来改善TBM的治疗结果,特别是关于高剂量利福平的价值、具有更好中枢神经系统穿透力的新型抗微生物药物以及宿主导向疗法。支持性措施,特别是合并HIV感染时脑积水的管理,应成为未来研究的一个领域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ae3f/5830467/67a1a6a1a838/11940_2018_490_Fig1_HTML.jpg

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