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‘ZS-MDR-TB versus ‘ZR-MDR-TB: improving treatment of MDR-TB by identifying pyrazinamide susceptibility

机译:ZS-MDR-TB与 ZR-MDR-TB:通过确定吡嗪酰胺敏感性来改善MDR-TB的治疗

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摘要

Indispensable for shortening treatment of drug-susceptible tuberculosis (TB), pyrazinamide (PZA, Z) is also essential in the treatment of multidrug-resistant (MDR)-TB. While resistance to PZA in MDR-TB is associated with poor treatment outcome, bacillary susceptibility to PZA along with the use of fluoroquinolone (FQ) and second-line injectable drugs (SLIDs) may predict improved treatment success in MDR-TB. Despite a high prevalence of PZA resistance among MDR-TB patients (10%–85%), PZA susceptibility testing is seldom performed because of technical challenges. To improve treatment of MDR-TB, we propose to: (i) classify MDR-TB into PZA-susceptible MDR-TB (ZS-MDR-TB) and PZA-resistant MDR-TB (ZR-MDR-TB); (ii) use molecular tests such as DNA sequencing (pncA, gyrA, rrs, etc.) to rapidly identify ZS-MDR-TB versus ZR-MDR-TB and susceptibility profile for FQ and SLID; (iii) refrain from using PZA in ZR-MDR-TB; and (iv) explore the feasibility of shortening the treatment duration of ZS-MDR-TB with a regimen comprising PZA plus at least two bactericidal agents especially new agents like TMC207 or PA-824 or delamanid which the bacilli are susceptible to, with one or two other agents. These measures may potentially shorten therapy, save costs, and reduce side effects of MDR-TB treatment.
机译:吡嗪酰胺(PZA,Z)对于缩短对药物敏感的结核(TB)的治疗必不可少,在治疗耐多药(MDR)-TB方面也必不可少。虽然耐多药结核病对PZA的耐药性与治疗效果差有关,但细菌对PZA的敏感性以及使用氟喹诺酮(FQ)和二线注射药物(SLIDs)可能预示了耐多药结核病治疗成功的改善。尽管耐多药结核病患者对PZA的耐药率很高(10%–85%),但由于技术挑战,很少进行PZA药敏试验。为了改善耐多药结核病的治疗,我们建议:(i)将耐多药结核病分为易感PZA的耐多药结核病(Z S -MDR-TB)和耐PZA的耐多药结核病(Z R -MDR-TB); (ii)使用诸如DNA测序(pncA,gyrA,rrs等)的分子测试来快速识别Z S -MDR-TB与Z R -MDR-TB FQ和SLID的敏感性分布; (iii)不要在Z R -MDR-TB中使用PZA; (iv)探讨采用PZA加至少两种杀菌剂,尤其是TMC207或PA-824或delamanid等新药来缩短Z S -MDR-TB治疗时间的可行性。细菌易与一种或两种其他药物感染。这些措施可能会缩短治疗时间,节省成本并减少耐多药结核病治疗的副作用。

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