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异烟肼和利福平耐药突变及其对二线抗结核治疗的影响。

Isoniazid and rifampicin resistance mutations and their effect on second-line anti-tuberculosis treatment.

作者信息

Abate D, Tedla Y, Meressa D, Ameni G

机构信息

<label>*</label>Aklilu Lemma Institute of Pathobiology, Addis Ababa University, Addis Ababa, Ethiopia.

<label><sup>†</sup></label>St Peter TB Specialised Hospital, Addis Ababa, Ethiopia.

出版信息

Int J Tuberc Lung Dis. 2014 Aug;18(8):946-51. doi: 10.5588/ijtld.13.0926.

Abstract

SETTING

St Peter's TB Specialized Hospital, Addis Ababa, Ethiopia.

OBJECTIVE

To estimate the prevalence of mutations that cause resistance to isoniazid (INH) and rifampicin (RMP) and assess the effects of these mutations on second-line anti-tuberculosis treatment.

DESIGN

GenoType(®)MTBDRplus assay results and clinical data documented at St Peter's TB Specialized Hospital over 3 years were retrospectively collected and analysed.

RESULTS

The results indicated that 68.7% (n = 470) of RMP-resistant isolates had mutations at codon 531 (S531L) of the rpoB gene, while 93% (n = 481) of the INH-resistant isolates had mutations at codon 315 (S315T1) of the katG gene. The proportion of inhA mutations was 0.8% (n = 481). Treatment outcome was unfavourable in 23.7% (n = 76) of patients treated with second-line anti-tuberculosis drugs. Mutations in other codons of the rpoB gene (P > 0.05) and in the inhA promoter region (P > 0.05) were not associated with unfavourable treatment outcomes.

CONCLUSION

The predominant mutations in RMP and INH resistance were observed at codons 531 and 315 in the rpoB and katG genes, respectively. Mutations in the inhA region were rare, which shows its minimal contribution to the development of resistance to ethionamide. This also suggests that treating multidrug-resistant TB patients with high doses of INH may have little effect.

摘要

背景

埃塞俄比亚亚的斯亚贝巴圣彼得结核病专科医院。

目的

评估导致对异烟肼(INH)和利福平(RMP)耐药的突变发生率,并评估这些突变对二线抗结核治疗的影响。

设计

回顾性收集并分析圣彼得结核病专科医院3年期间记录的GenoType(®)MTBDRplus检测结果和临床数据。

结果

结果表明,68.7%(n = 470)的利福平耐药菌株在rpoB基因的531密码子(S531L)处发生突变,而93%(n = 481)的异烟肼耐药菌株在katG基因的315密码子(S315T1)处发生突变。inhA基因突变的比例为0.8%(n = 481)。接受二线抗结核药物治疗的患者中,23.7%(n = 76)的治疗结果不佳。rpoB基因其他密码子(P > 0.05)和inhA启动子区域(P > 0.05)的突变与不良治疗结果无关。

结论

分别在rpoB基因的531密码子和katG基因的315密码子处观察到利福平和异烟肼耐药的主要突变。inhA区域的突变很少见,这表明其对乙硫异烟胺耐药性发展的贡献最小。这也表明,用高剂量异烟肼治疗耐多药结核病患者可能效果甚微。

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