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首次记录结核分枝杆菌异烟肼耐药逆转。

First documentation of isoniazid reversion in Mycobacterium tuberculosis.

机构信息

Department of Pathology, Stanford University School of Medicine, Stanford, California, USA.

出版信息

Int J Tuberc Lung Dis. 2009 Nov;13(11):1347-54.

Abstract

BACKGROUND

Drug-resistant strains of Mycobacterium tuberculosis are increasing worldwide and pose a major threat to global health. However, it remains unsettled whether drug-resistant mutants are fixed in the bacterial population or if they would revert in the absence of drug pressure.

OBJECTIVE

To document the occurrence of isoniazid (INH) reversion in a patient with multidrug-resistant tuberculosis (TB) and investigate its association with fitness cost.

DESIGN

Genotypic and phenotypic assays were used to characterize the reversion of INH resistance in isolates from a patient with pulmonary TB. The pre-reversion katG mutation was reconstructed in a pan-susceptible laboratory strain (H37Rv DeltakatG::katG W300G) and tested for susceptibility to INH and oxidative stress.

RESULTS

Genotyping and drug susceptibility testing showed that an isogenic strain of M. tuberculosis reverted from an INH-resistant to a susceptible phenotype in the absence of INH therapy. The genotypic basis of this reversion was mapped to the katG codon 300 which reverted from GGG (glycine, G) to a wild-type codon, TGG (tryptophan, W). The H37Rv DeltakatG::katG W300G mutant was resistant to INH, but also showed a deficiency in coping with oxidative stress.

CONCLUSION

This study confirms that, in the absence of INH pressure, some INH-resistant mutants will revert to a drug-susceptible phenotype. This finding may have broader implications for INH-resistant strains and for the clinically useful lifespan of INH.

摘要

背景

全球范围内耐多药结核分枝杆菌(Mycobacterium tuberculosis)耐药株不断增加,对全球健康构成重大威胁。然而,耐药突变体是否在细菌群体中固定下来,或者在没有药物压力的情况下是否会回复,仍未得到解决。

目的

记录耐多药结核病(TB)患者中异烟肼(INH)回复的发生情况,并探讨其与适应性成本的关系。

设计

使用基因型和表型检测方法来描述来自患有肺结核患者的分离物中 INH 耐药性的回复情况。在泛敏感实验室菌株(H37Rv DeltakatG::katG W300G)中重建了前回复 katG 突变,并测试了对 INH 和氧化应激的敏感性。

结果

基因分型和药敏试验表明,在没有 INH 治疗的情况下,一株结核分枝杆菌同基因株从 INH 耐药表型回复为敏感表型。这种回复的基因型基础被映射到 katG 密码子 300 上,该密码子从 GGG(甘氨酸,G)回复为野生型密码子,TGG(色氨酸,W)。H37Rv DeltakatG::katG W300G 突变体对 INH 耐药,但也显示出应对氧化应激的缺陷。

结论

本研究证实,在没有 INH 压力的情况下,一些 INH 耐药突变体将回复为药物敏感表型。这一发现可能对 INH 耐药株以及 INH 的临床有效寿命具有更广泛的意义。

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