Acquisition of Cross-Resistance to Bedaquiline and Clofazimine following Treatment for Tuberculosis in Pakistan

Ghodousi, Arash; Rizvi, Alamdar Hussain; Baloch, Aurangzaib Quadir; Ghafoor, Abdul; Khanzada, Faisal Masood; Qadir, Mehmood; Borroni, Emanuele; Trovato, Alberto; Tahseen, Sabira; Cirillo, Daniela María

doi:10.1128/aac.00915-19

Cited by 55 publications

(47 citation statements)

References 12 publications

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“…Thus, the role of the Rv0678 and atpE in resistance is controversial, as mutations of these genes in susceptible and resistant strains have been reported. In other words, both susceptible and BDQ-resistant strains may carry mutations in these genes and the presence of mutations does not necessarily indicate resistance [32,63,64].…”

Section: Discussionmentioning

confidence: 99%

Whole Genome Sequencing Results Associated with Minimum Inhibitory Concentrations of 14 Anti-Tuberculosis Drugs among Rifampicin-Resistant Isolates of Mycobacterium Tuberculosis from Iran

Kardan-Yamchi

Kazemian

Battaglia

et al. 2020

JCM

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Accurate and timely detection of drug resistance can minimize the risk of further resistance development and lead to effective treatment. The aim of this study was to determine the resistance to first/second-line anti-tuberculosis drugs in rifampicin/multidrug-resistant Mycobacterium tuberculosis (RR/MDR-MTB) isolates. Molecular epidemiology of strains was determined using whole genome sequencing (WGS)-based genotyping. A total of 35 RR/MDR-MTB isolates were subjected to drug susceptibility testing against first/second-line drugs using 7H9 Middlebrook in broth microdilution method. Illumina technology was used for paired-end WGS applying a Maxwell 16 Cell DNA Purification kit and the NextSeq platform. Data analysis and single nucleotide polymorphism calling were performed using MTBseq pipeline. The genome-based resistance to each drug among the resistant phenotypes was as follows: rifampicin (97.1%), isoniazid (96.6%), ethambutol (100%), levofloxacin (83.3%), moxifloxacin (83.3%), amikacin (100%), kanamycin (100%), capreomycin (100%), prothionamide (100%), D-cycloserine (11.1%), clofazimine (20%), bedaquiline (0.0%), and delamanid (44.4%). There was no linezolid-resistant phenotype, and a bedaquiline-resistant strain was wild type for related genes. The Beijing, Euro-American, and Delhi-CAS were the most populated lineage/sublineages. Drug resistance-associated mutations were mostly linked to minimum inhibitory concentration results. However, the role of well-known drug-resistant genes for D-cycloserine, clofazimine, bedaquiline, and delamanid was found to be more controversial.

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Section: Discussionmentioning

confidence: 99%

Whole Genome Sequencing Results Associated with Minimum Inhibitory Concentrations of 14 Anti-Tuberculosis Drugs among Rifampicin-Resistant Isolates of Mycobacterium Tuberculosis from Iran

Kardan-Yamchi

Kazemian

Battaglia

et al. 2020

JCM

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“…The proposed combination may jeopardize treatment options for those patients, particularly if failure strains are resistant to both second-line core drugs: bedaquiline and FLQ [37]. Indeed, some small studies of bedaquiline-containing regimens show high rates of acquired drug resistance to bedaquiline: 24 out of 116 tests in Russia [38], and 6 out of 30 in Pakistan [39]. An alternative approach, applying the cascade of regimens concept, seems a better option: in TB treatment regimens, the core drug should be rifampicin when the strain is susceptible to rifampicin, a later generation FLQ in case of resistance to rifampicin, and bedaquiline if there is a resistance to FLQ [14].…”

Section: Discussionmentioning

confidence: 99%

Short-Course Regimen for Multidrug-Resistant Tuberculosis: A Decade of Evidence

Trébucq

Decroo

Deun

et al. 2019

JCM

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About ten years ago, the first results of the so-called “Bangladesh regimen”, a short regimen lasting nine months instead of 20 months, revolutionized multidrug-resistant tuberculosis (MDR-TB) treatment. Similar short regimens were studied in different settings, relying for their efficacy on a later generation fluoroquinolone, either gatifloxacin, moxifloxacin, or levofloxacin. We review the published material on short MDR-TB regimens, describe their different compositions, their results in national tuberculosis programs in middle- and low-income countries, the risk of acquiring resistance to fluoroquinolone, and the occurrence of adverse events. With over 80% success, the regimen performs much better than longer regimens (usually around 50%). Monitoring of adverse events allows adapting its composition to prevent severe adverse events such as deafness. We discuss the current applicability and usefulness of the short injectable-containing regimen given the 2019 recommendation of the World Health Organization (WHO) for a new long all-oral regimen. We conclude that the most effective fluoroquinolone is gatifloxacin, currently not listed as an essential medicine by WHO. It is a priority to restore its status as an essential medicine.

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“…However, our phenotypic and in silico results suggest that Leu117Arg affects the dimerization of Rv0678 causing a small increase but not high-level value of BDQ MIC. Other mutations in Rv0678 were described at the same codon position but with a different amino acid change ( 5, 8, 9, 11, 13 ). The Rv0678 mutations Val20Phe, Ala84Glu and Arg90Pro were observed to be linked to increase MICs for CLF and potentially associated to a BDQ-resistant phenotype, while Val20Gly was associated with both BDQ and CLF resistance ( 5, 9 ).…”

Section: Discussionmentioning

confidence: 99%

“…Other mutations in Rv0678 were described at the same codon position but with a different amino acid change ( 5, 8, 9, 11, 13 ). The Rv0678 mutations Val20Phe, Ala84Glu and Arg90Pro were observed to be linked to increase MICs for CLF and potentially associated to a BDQ-resistant phenotype, while Val20Gly was associated with both BDQ and CLF resistance ( 5, 9 ). In this study, Rv0678 mutations Val20Ala and Ala84Val were found in BDQ-susceptible strains (MIC ≤ 0.008 µg/ml), while Arg90Cys was associated with a BDQ MIC value of 0.12 µg/ml.…”

Section: Discussionmentioning

confidence: 99%

“…Based on WHO priority grouping of medicines, Delamanid (DLM) compound is recommended when an effective regimen cannot be established by group A agents, containing BDQ, fluoroquinolones (FQs), linezolid (LZD) and B agents group, composed by clofazimine (CLF) and cycloserine (CS) ( 2 ). Previous studies have shown that MDR/XDR-TB patients treated with BDQ and DLM rapidly develop resistance due to fixed mutations in candidate genes which often appear as previously undescribed novel variants ( 3, 4, 5, 6, 7 ). Additionally, resistance to BDQ can arise in naïve populations of MTBc strains as a consequence of a clofazimine-containing regimen, or by random mutations affecting the drug targets ( 8, 9, 10, 11, 12, 13, 14 ).…”

Section: Introductionmentioning

confidence: 99%

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Characterization of genomic variants associated with resistance to bedaquiline and delamanid in naïve Mycobacterium tuberculosis clinical strains

Battaglia¹,

Spitaleri

Cabibbe³

et al. 2020

Preprint

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The role of genetic mutations in genes associated to phenotypic resistance to bedaquiline (BDQ) and delamanid (DLM) in Mycobacterium tuberculosis complex (MTBc) strains is poorly understood. However, a clear understanding of the role of each genetic variant is crucial to guide the development of molecular-based drug susceptibility testing (DST). In this work, we analysed all mutations in candidate genomic regions associated with BDQ- and DLM-resistant phenotypes using a whole genome sequencing (WGS) dataset from a collection of 4795 MTBc clinical isolates from six high-burden countries of tuberculosis (TB). From WGS analysis, we identified 61 and 158 unique mutations in genomic regions potentially involved in BDQ- and DLM-resistant phenotypes, respectively. Importantly, all strains were isolated from patients who likely have never been exposed to the medicines. In order to characterize the role of mutations, we performed an energetic in silico analysis to evaluate their effect in the available protein structures Ddn (DLM), Fgd1 (DLM) and Rv0678 (BDQ), and minimum inhibitory concentration (MIC) assays on a subset of MTBc strains carrying mutations to assess their phenotypic effect. The combination of structural protein information and phenotypic data allowed for cataloging the mutations clearly associated with resistance to BDQ (n= 4) and DLM (n= 35), as well as about a hundred genetic variants without any correlation with resistance. Importantly, these results show that both BDQ and DLM resistance-related mutations are diverse and distributed across the entire region of each gene target, which is of critical importance to the development of comprehensive molecular diagnostic tools.ImportancePhenotypic drug susceptibility tests (DST) are too slow to provide an early indication of drug susceptibility status at the time of treatment initiation and very demanding in terms of specimens handling and biosafety. The development of molecular assays to detect resistance to bedaquiline (BDQ) and delamanid (DLM) requires accurate categorization of genetic variants according to their association with phenotypic resistance. We have evaluated a large multi-country set of clinical isolates to identify mutations associated with increased minimum inhibitory concentrations (MICs) and used an in silico protein structure analysis to further unravel the potential role of these mutations in drug resistance mechanisms. The results of this study are an important source of information for the development of molecular diagnostic tests to improve the provision of appropriate treatment and care to TB patients.

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Acquisition of Cross-Resistance to Bedaquiline and Clofazimine following Treatment for Tuberculosis in Pakistan

Cited by 55 publications

References 12 publications

Whole Genome Sequencing Results Associated with Minimum Inhibitory Concentrations of 14 Anti-Tuberculosis Drugs among Rifampicin-Resistant Isolates of Mycobacterium Tuberculosis from Iran

Whole Genome Sequencing Results Associated with Minimum Inhibitory Concentrations of 14 Anti-Tuberculosis Drugs among Rifampicin-Resistant Isolates of Mycobacterium Tuberculosis from Iran

Short-Course Regimen for Multidrug-Resistant Tuberculosis: A Decade of Evidence

Characterization of genomic variants associated with resistance to bedaquiline and delamanid in naïve Mycobacterium tuberculosis clinical strains

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