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结核病主动病例发现中成本与准确性之间的权衡:动态建模分析

Trade-offs between cost and accuracy in active case finding for tuberculosis: A dynamic modelling analysis.

作者信息

Cilloni Lucia, Kranzer Katharina, Stagg Helen R, Arinaminpathy Nimalan

机构信息

MRC Centre for Global Infectious Disease Analysis, School of Public Health, Imperial College London, London, United Kingdom.

Clinical Research Department, London School of Hygiene & Tropical Medicine, London, United Kingdom.

出版信息

PLoS Med. 2020 Dec 2;17(12):e1003456. doi: 10.1371/journal.pmed.1003456. eCollection 2020 Dec.

Abstract

BACKGROUND

Active case finding (ACF) may be valuable in tuberculosis (TB) control, but questions remain about its optimum implementation in different settings. For example, smear microscopy misses up to half of TB cases, yet is cheap and detects the most infectious TB cases. What, then, is the incremental value of using more sensitive and specific, yet more costly, tests such as Xpert MTB/RIF in ACF in a high-burden setting?

METHODS AND FINDINGS

We constructed a dynamic transmission model of TB, calibrated to be consistent with an urban slum population in India. We applied this model to compare the potential cost and impact of 2 hypothetical approaches following initial symptom screening: (i) 'moderate accuracy' testing employing a microscopy-like test (i.e., lower cost but also lower accuracy) for bacteriological confirmation and (ii) 'high accuracy' testing employing an Xpert-like test (higher cost but also higher accuracy, while also detecting rifampicin resistance). Results suggest that ACF using a moderate-accuracy test could in fact cost more overall than using a high-accuracy test. Under an illustrative budget of US$20 million in a slum population of 2 million, high-accuracy testing would avert 1.14 (95% credible interval 0.75-1.99, with p = 0.28) cases relative to each case averted by moderate-accuracy testing. Test specificity is a key driver: High-accuracy testing would be significantly more impactful at the 5% significance level, as long as the high-accuracy test has specificity at least 3 percentage points greater than the moderate-accuracy test. Additional factors promoting the impact of high-accuracy testing are that (i) its ability to detect rifampicin resistance can lead to long-term cost savings in second-line treatment and (ii) its higher sensitivity contributes to the overall cases averted by ACF. Amongst the limitations of this study, our cost model has a narrow focus on the commodity costs of testing and treatment; our estimates should not be taken as indicative of the overall cost of ACF. There remains uncertainty about the true specificity of tests such as smear and Xpert-like tests in ACF, relating to the accuracy of the reference standard under such conditions.

CONCLUSIONS

Our results suggest that cheaper diagnostics do not necessarily translate to less costly ACF, as any savings from the test cost can be strongly outweighed by factors including false-positive TB treatment, reduced sensitivity, and foregone savings in second-line treatment. In resource-limited settings, it is therefore important to take all of these factors into account when designing cost-effective strategies for ACF.

摘要

背景

主动病例发现(ACF)在结核病(TB)控制中可能具有重要价值,但在不同环境中其最佳实施方式仍存在疑问。例如,涂片显微镜检查会漏诊高达一半的结核病病例,但其成本低廉且能检测出传染性最强的结核病病例。那么,在高负担环境下的ACF中,使用更敏感、特异但成本更高的检测方法(如Xpert MTB/RIF)的增量价值是什么呢?

方法与结果

我们构建了一个结核病动态传播模型,并根据印度城市贫民窟人口进行校准。我们应用该模型比较了初始症状筛查后两种假设方法的潜在成本和影响:(i)采用类似显微镜检查的“中等准确性”检测(即成本较低但准确性也较低)进行细菌学确认;(ii)采用类似Xpert的检测(成本较高但准确性也较高,同时还能检测利福平耐药性)进行“高准确性”检测。结果表明,使用中等准确性检测的ACF实际上总体成本可能高于使用高准确性检测。在一个有200万人口的贫民窟,预算为2000万美元的情况下,相对于中等准确性检测避免的每例病例,高准确性检测将避免1.14例(95%可信区间为0.75 - 1.99,p = 0.28)。检测特异性是一个关键驱动因素:只要高准确性检测的特异性比中等准确性检测至少高3个百分点,在5%的显著性水平下,高准确性检测的影响将显著更大。促进高准确性检测影响的其他因素包括:(i)其检测利福平耐药性的能力可导致二线治疗的长期成本节约;(ii)其更高的敏感性有助于ACF避免的总体病例数增加。本研究的局限性包括,我们的成本模型仅关注检测和治疗的商品成本;我们的估计不应被视为ACF总体成本的指标。在ACF中,涂片和类似Xpert检测等检测方法的真正特异性仍存在不确定性,这与在此类条件下参考标准的准确性有关。

结论

我们的结果表明,成本较低的诊断方法不一定意味着ACF成本更低,因为检测成本的任何节省可能会被包括假阳性结核病治疗、敏感性降低以及二线治疗中节省的损失等因素大大超过。因此,在资源有限的环境中,设计具有成本效益的ACF策略时,考虑所有这些因素非常重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8148/7710036/fb840824bfab/pmed.1003456.g001.jpg

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