Activity of phenothiazines against antibiotic-resistant Mycobacterium tuberculosis: a review supporting further studies that may elucidate the potential use of thioridazine as anti-tuberculosis therapy

doi:10.1093/jac/47.5.505

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Journal of Antimicrobial Chemotherapy (2001) 47, 505-511
© 2001 The British Society for Antimicrobial Chemotherapy

Review

Activity of phenothiazines against antibiotic-resistant Mycobacterium tuberculosis: a review supporting further studies that may elucidate the potential use of thioridazine as anti-tuberculosis therapy

Leonard Amaral^a^,*, Jette E. Kristiansen^b, Miguel Viveiros^a and Jorge Atouguia^c

^a Unit of Mycobacteriology and ^c Unit of Clinics of Tropical Diseases, Institute of Hygiene and Tropical Medicine, Universidade Nova de Lisboa, Lisbon, Portugal; ^b Department of Microbiology, Sonderborg Sygehus, Sonderborg, Denmark

The in vitro and in vivo anti-mycobacterial activities of anumber of phenothiazine compounds are reviewed. These compounds,normally employed for the management of psychosis, inhibit thegrowth in vitro of Mycobacterium tuberculosis at concentrationsthat are significantly greater than those that can safely beachieved in a patient harbouring these infections. Nevertheless,one of these phenothiazines, chlorpromazine, is concentratedby human macrophages to 10–100 times its concentrationin plasma, and has activity against mycobacteria that have beenphagocytosed by these cells. Phenothiazines have significantin vitro activity against susceptible, polydrug- and multidrug-resistantstrains of M. tuberculosis, as well as enhancing the activityof some agents employed for first-line treatment. Because thioridazine,the very mild anti-psychotic agent whose most common side effectis drowsiness, has equal anti-tuberculosis properties in vitroto chlorpromazine, we recommend that thioridazine be studiedas an adjuvant to the four- or five-drug regimens employed forthe management of a freshly diagnosed tuberculosis infectionof unknown antibiotic susceptibility, at least during the periodrequired for the assessment of antibiotic susceptibility. Becauseit also enhances the activity of rifampicin and streptomycin,antibiotics that frequently have adverse effects, additionalstudies evaluating the use of thioridazine as an adjuvant mayeventually allow a reduction in the dosages of these antibioticsand result in a decreased frequency of adverse effects. It isimportant to note that whereas the management of patients withthioridazine for periods in excess of many months will resultin the appearance of some undesirable side effects, its usefor a limited period of 2–3 months should not produceside effects that are more severe than simple drowsiness. Nevertheless,further in vitro and in vivo studies are essential before thioridazinemay be recommended for the management of select cases of pulmonarytuberculosis.

^* Correspondence address. Instituto de Higiene e Medicina Tropical,Universidade Nova de Lisboa, Rua Junqueira 96, 1349-008 Lisbon,Portugal. Tel: +351-21-365-26-53; Fax: +351-21-363-21-05; E-mail:lamaral{at}ihmt.unl.pt

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