TY - JOUR KW - Antitubercular Agents KW - Bacterial Proteins KW - Crystallography, X-Ray KW - Drug Design KW - Drug Resistance, Multiple, Bacterial KW - Ethionamide KW - Humans KW - In Vitro Techniques KW - Leprostatic Agents KW - leprosy KW - Models, Molecular KW - Mycobacterium avium Complex KW - Mycobacterium avium-intracellulare Infection KW - Mycobacterium leprae KW - Mycobacterium tuberculosis KW - NAD KW - Oxidoreductases KW - Prothionamide KW - Tuberculosis KW - Tuberculosis, Multidrug-Resistant AU - Wang F AU - Langley R AU - Gulten G AU - Dover LG AU - Besra G AU - Jacobs W AU - Sacchettini JC AB -

Thioamide drugs, ethionamide (ETH) and prothionamide (PTH), are clinically effective in the treatment of Mycobacterium tuberculosis, M. leprae, and M. avium complex infections. Although generally considered second-line drugs for tuberculosis, their use has increased considerably as the number of multidrug resistant and extensively drug resistant tuberculosis cases continues to rise. Despite the widespread use of thioamide drugs to treat tuberculosis and leprosy, their precise mechanisms of action remain unknown. Using a cell-based activation method, we now have definitive evidence that both thioamides form covalent adducts with nicotinamide adenine dinucleotide (NAD) and that these adducts are tight-binding inhibitors of M. tuberculosis and M. leprae InhA. The crystal structures of the inhibited M. leprae and M. tuberculosis InhA complexes provide the molecular details of target-drug interactions. The purified ETH-NAD and PTH-NAD adducts both showed nanomolar Kis against M. tuberculosis and M. leprae InhA. Knowledge of the precise structures and mechanisms of action of these drugs provides insights into designing new drugs that can overcome drug resistance.

BT - The Journal of experimental medicine C1 - http://www.ncbi.nlm.nih.gov/pubmed/17227913?dopt=Abstract DA - 2007 Jan 22 DO - 10.1084/jem.20062100 IS - 1 J2 - J. Exp. Med. LA - eng N2 -

Thioamide drugs, ethionamide (ETH) and prothionamide (PTH), are clinically effective in the treatment of Mycobacterium tuberculosis, M. leprae, and M. avium complex infections. Although generally considered second-line drugs for tuberculosis, their use has increased considerably as the number of multidrug resistant and extensively drug resistant tuberculosis cases continues to rise. Despite the widespread use of thioamide drugs to treat tuberculosis and leprosy, their precise mechanisms of action remain unknown. Using a cell-based activation method, we now have definitive evidence that both thioamides form covalent adducts with nicotinamide adenine dinucleotide (NAD) and that these adducts are tight-binding inhibitors of M. tuberculosis and M. leprae InhA. The crystal structures of the inhibited M. leprae and M. tuberculosis InhA complexes provide the molecular details of target-drug interactions. The purified ETH-NAD and PTH-NAD adducts both showed nanomolar Kis against M. tuberculosis and M. leprae InhA. Knowledge of the precise structures and mechanisms of action of these drugs provides insights into designing new drugs that can overcome drug resistance.

PY - 2007 SP - 73 EP - 8 T2 - The Journal of experimental medicine TI - Mechanism of thioamide drug action against tuberculosis and leprosy. VL - 204 SN - 0022-1007 ER -