Genome-wide analysis of multi- and extensively drug-resistant $Mycobacterium\ tuberculosis$

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Coll, Francesc | Phelan, Jody | Hill-Cawthorne, Grant | Nair, Mridul | Mallard, Kim | Ali, Shahjahan | Abdallah, Abdallah | Alghamdi, Saad | Alsomali, Mona | Ahmed, Abdallah | Portelli, Stephanie | Oppong, Yaa | Alves, Adriana | Bessa, Theolis Barbosa | Campino, Susana | Caws, Maxine | Chatterjee, Anirvan | Crampin, Amelia | Dheda, Keertan | Furnham, Nicholas | Glynn, Judith | Grandjean, Louis | Minh Ha, Dang | Hasan, Rumina | Hasan, Zahra | Hibberd, Martin, L | Joloba, Moses | Jones-López, Edward | Matsumoto, Tomoshige | Miranda, Anabela | Moore, David | Mocillo, Nora | Panaiotov, Stefan | Parkhill, Julian | Penha, Carlos | Perdigão, João | Portugal, Isabel | Rchiad, Zineb | Robledo, Jaime | Sheen, Patricia | Shesha, Nashwa Talaat | Sirgel, Frik | Sola, Christophe | Oliveira Sousa, Erivelton | Streicher, Elizabeth | Helden, Paul Van | Viveiros, Miguel | Warren, Robert | Mcnerney, Ruth | Pain, Arnab | Clark, Taane

Edité par CCSD ; Nature Publishing Group -

International audience. To characterize the genetic determinants of resistance to antituberculosis drugs, we performed a genome-wide association study (GWAS) of 6,465 $Mycobacterium\ tuberculosis$ clinical isolates from more than 30 countries. A GWAS approach within a mixed-regression framework was followed by a phylogenetics-based test for independent mutations. In addition to mutations in established and recently described resistance-associated genes, novel mutations were discovered for resistance to cycloserine, ethionamide and para-aminosalicylic acid. The capacity to detect mutations associated with resistance to ethionamide, pyrazinamide, capreomycin, cycloserine and para-aminosalicylic acid was enhanced by inclusion of insertions and deletions. Odds ratios for mutations within candidate genes were found to reflect levels of resistance. New epistatic relationships between candidate drug-resistance-associated genes were identified. Findings also suggest the involvement of efflux pumps ($drrA$ and $Rv2688c$) in the emergence of resistance. This study will inform the design of new diagnostic tests and expedite the investigation of resistance and compensatory epistatic mechanisms.

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