采用 9 个月方案治疗耐多药结核病的预期效果:基于人群的建模分析。
Expected effects of adopting a 9 month regimen for multidrug-resistant tuberculosis: a population modelling analysis.
机构信息
Division of Infectious Diseases, Johns Hopkins University School of Medicine, Baltimore, MD, USA.
Division of General Internal Medicine, Johns Hopkins University School of Medicine, Baltimore, MD, USA.
出版信息
Lancet Respir Med. 2017 Mar;5(3):191-199. doi: 10.1016/S2213-2600(16)30423-4. Epub 2016 Dec 16.
BACKGROUND
In May, 2016, WHO endorsed a 9 month regimen for multidrug-resistant tuberculosis that is cheaper and potentially more effective than the conventional, longer (20-24 month) therapy. We aimed to investigate the population-level implications of scaling up this new regimen.
METHODS
In this population modelling analysis, we developed a dynamic transmission model to simulate the introduction of this short-course regimen as an instantaneous switch in 2016. We projected the corresponding percentage reduction in the incidence of multidrug-resistant tuberculosis by 2024 compared with continued use of longer therapy. In the primary analysis in a representative southeast Asian setting, we assumed that the short-course regimen would double treatment access (through savings in resources or capacity) and achieve long-term efficacy at levels seen in preliminary cohort studies. We then did extensive sensitivity analyses to explore a range of alternative scenarios.
FINDINGS
Under the optimistic assumptions in the primary analysis, the incidence of multidrug-resistant tuberculosis in 2024 would be 3·3 (95% uncertainty range 2·2-5·6) per 100 000 population with the short-course regimen and 4·3 (2·9-7·6) per 100 000 population with continued use of longer therapy-ie, the short-course regimen could reduce incidence by 23% (10-38). Incidence would be reduced by 14% (4-28) if the new regimen affected only treatment effectiveness and by 11% (3-24) if it affected only treatment availability. Under more pessimistic assumptions, the short-course regimen would have minimal effect and even potential for harm-eg, when 30% of patients are ineligible for the new regimen because of second-line drug resistance, we projected a change in incidence of -2% (-20 to +28). The new regimen's effect was greater in settings with more ongoing transmission of multidrug-resistant tuberculosis, but results were otherwise similar across settings with different levels of tuberculosis incidence and prevalence of multidrug resistance.
INTERPRETATION
The short-course regimen has potential to substantially lessen the multidrug-resistant tuberculosis epidemic, but this effect depends on its long-term efficacy, its ability to expand treatment access, and the role of second-line drug resistance.
FUNDING
US National Institutes of Health and Bill & Melinda Gates Foundation.
背景
2016 年 5 月,世界卫生组织(WHO)认可了一种 9 个月疗程的耐多药结核病治疗方案,该方案比传统的、更长(20-24 个月)疗程的治疗方案更便宜,且潜在效果更好。我们旨在研究扩大这一新方案的人群层面的影响。
方法
在这项基于人群的模型分析中,我们开发了一个动态传播模型,以模拟 2016 年瞬间切换使用这种短程方案的情况。我们预测了与继续使用长程治疗相比,到 2024 年耐多药结核病发病率的相应降低百分比。在具有代表性的东南亚环境中的主要分析中,我们假设短程方案将通过节省资源或能力使治疗机会增加一倍,并实现初步队列研究中观察到的长期疗效。然后,我们进行了广泛的敏感性分析,以探索一系列替代方案。
结果
在主要分析中的乐观假设下,采用短程方案的 2024 年耐多药结核病发病率为 3.3(95%置信区间 2.2-5.6)/100000 人,而继续使用长程治疗的发病率为 4.3(2.9-7.6)/100000 人,即短程方案可将发病率降低 23%(10-38)。如果新方案仅影响治疗效果,则发病率降低 14%(4-28);如果仅影响治疗的可及性,则发病率降低 11%(3-24)。在更悲观的假设下,短程方案效果甚微,甚至可能产生危害,例如,如果由于二线药物耐药性,有 30%的患者不符合新方案的条件,我们预计发病率的变化为-2%(-20 至 +28)。在耐多药结核病传播率较高的环境中,新方案的效果更大,但在不同结核病发病率和耐多药耐药率的环境中,结果基本相似。
解释
短程方案有可能大大减轻耐多药结核病的流行,但这取决于其长期疗效、扩大治疗机会的能力以及二线药物耐药性的作用。
资助
美国国立卫生研究院和比尔及梅琳达·盖茨基金会。
Zotero 插件