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Modelling the effect of short-course multidrug-resistant tuberculosis treatment in Karakalpakstan, Uzbekistan

James M. TrauerSchool of Public Health and Preventive Medicine, Monash University, Melbourne, Australia. [email protected]Jay AcharMédecins sans Frontières, Manson Unit, London, UKNargiza ParpievaNational TB Institute, Ministry of Health, Tashkent, UzbekistanAtadjan KhamraevMinistry of Health, Nukus, UzbekistanJustin T. DenholmThe Victorian Tuberculosis Program at the Peter Doherty Institute, Melbourne, AustraliaDennis FalzonGlobal TB Programme, World Health Organization, Geneva, SwitzerlandErnesto JaramilloGlobal TB Programme, World Health Organization, Geneva, SwitzerlandAnita MesićMédecins sans Frontières Holland, Amsterdam, The NetherlandsPhilipp du CrosMédecins sans Frontières, Manson Unit, London, UKEmma S. McBrydeJames Cook University, Queensland, Australia
BMC Medicinejournal2016en
ABI

Аннотация

BACKGROUND: Multidrug-resistant tuberculosis (MDR-TB) is a major threat to global TB control. MDR-TB treatment regimens typically have a high pill burden, last 20 months or more and often lead to unsatisfactory outcomes. A 9-11 month regimen with seven antibiotics has shown high success rates among selected MDR-TB patients in different settings and is conditionally recommended by the World Health Organization. METHODS: We construct a transmission-dynamic model of TB to estimate the likely impact of a shorter MDR-TB regimen when applied in a low HIV prevalence region of Uzbekistan (Karakalpakstan) with high rates of drug resistance, good access to diagnostics and a well-established community-based MDR-TB treatment programme providing treatment to around 400 patients. The model incorporates acquisition of additional drug resistance and incorrect regimen assignment. It is calibrated to local epidemiology and used to compare the impact of shorter treatment against four alternative programmatic interventions. RESULTS: Based on empirical outcomes among MDR-TB patients and assuming no improvement in treatment success rates, the shorter regimen reduced MDR-TB incidence from 15.2 to 9.7 cases per 100,000 population per year and MDR-TB mortality from 3.0 to 1.7 deaths per 100,000 per year, achieving comparable or greater gains than the alternative interventions. No significant increase in the burden of higher levels of resistance was predicted. Effects are probably conservative given that the regimen is likely to improve success rates. CONCLUSIONS: In addition to benefits to individual patients, we find that shorter MDR-TB treatment regimens also have the potential to reduce transmission of resistant strains. These findings are in the epidemiological setting of treatment availability being an important bottleneck due to high numbers of patients being eligible for treatment, and may differ in other contexts. The high proportion of MDR-TB with additional antibiotic resistance simulated was not exacerbated by programmatic responses and greater gains may be possible in contexts where the regimen is more widely applicable.

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