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Adjunctive use of celecoxib with anti-tuberculosis drugs: evaluation in a whole-blood bactericidal activity model.


ABSTRACT: COX-2 inhibition may be of benefit in the treatment of tuberculosis (TB) through a number of pathways including efflux pump inhibition (increasing intracellular TB drug levels) and diverse effects on inflammation and the immune response. We investigated celecoxib (a COX-2 inhibitor) alone and with standard anti-tuberculosis drugs in the whole-blood bactericidal activity (WBA) model. Healthy volunteers took a single dose of celecoxib (400?mg), followed (after 1 week) by a single dose of either rifampicin (10?mg/kg) or pyrazinamide (25?mg/kg), followed (after 2 or 7 days respectively) by the same anti-tuberculosis drug with celecoxib. WBA was measured at intervals until 8?hours post-dose (by inoculating blood samples with Mycobacterium tuberculosis and estimating the change in bacterial colony forming units after 72?hours incubation). Celecoxib had no activity alone in the WBA assay (cumulative WBA over 8?hours post-dose: 0.03?±?0.01?logCFU, p?=?1.00 versus zero). Celecoxib did not increase cumulative WBA of standard TB drugs (mean cumulative WBA -0.10?±?0.13?logCFU versus -0.10?±?0.12?logCFU for TB drugs alone versus TB drugs and celecoxib; mean difference -0.01, 95% CI -0.02 to 0.00; p?=?0.16). The lack of benefit of celecoxib suggests that efflux pump inhibition or eicosanoid pathway-related responses are of limited importance in mycobacterial killing in the WBA assay.

SUBMITTER: Naftalin CM 

PROVIDER: S-EPMC6131161 | biostudies-literature | 2018 Sep

REPOSITORIES: biostudies-literature

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Adjunctive use of celecoxib with anti-tuberculosis drugs: evaluation in a whole-blood bactericidal activity model.

Naftalin Claire M CM   Verma Rupangi R   Gurumurthy Meera M   Hee Kim Hor KH   Lu Qingshu Q   Yeo Benjamin Chaik Meng BCM   Tan Kin Hup KH   Lin Wenwei W   Yu Buduo B   Seng Kok Yong KY   Lee Lawrence Soon-U LS   Paton Nicholas I NI  

Scientific reports 20180910 1


COX-2 inhibition may be of benefit in the treatment of tuberculosis (TB) through a number of pathways including efflux pump inhibition (increasing intracellular TB drug levels) and diverse effects on inflammation and the immune response. We investigated celecoxib (a COX-2 inhibitor) alone and with standard anti-tuberculosis drugs in the whole-blood bactericidal activity (WBA) model. Healthy volunteers took a single dose of celecoxib (400 mg), followed (after 1 week) by a single dose of either ri  ...[more]

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