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15 May 2005

Volume 40, Number 10
Clinical Infectious Diseases 2005;40:1395–1403
© 2005 by the Infectious Diseases Society of America. All rights rwerved.
1058-4838/2005/4010-0003$15.00
DOI: 10.1086/429238
MAJOR ARTICLE

Randomized, Double‐Blind Clinical Trial of Topical Imiquimod 5% with Parenteral Meglumine Antimoniate in the Treatment of Cutaneous Leishmaniasis in Peru

C. Miranda‐Verástegui,1,3

A. Llanos‐Cuentas,3

I. Arévalo,1

B.J. Ward,2 and

G. Matlashewski1

1Department of Microbiology and Immunology, McGill University, and 2McGill Centre for Tropical Diseases, McGill University Health Center, Montreal, Canada; and 3Instituto de Medicina Tropical Alexander von Humbolt, Universidad Peruana Cayetano Heredia, Lima, Perú

Background.Current treatments for cutaneous leishmaniasis are limited by their toxicity, high cost, and discomfort and the emergence of drug resistance. New approaches, including combination therapies, are urgently needed. We performed a double‐blind, randomized trial of therapy with parenteral antimony plus topical imiquimod, an innate immune–response modulator, versus therapy with antimony alone, in subjects with cutaneous leishmaniasis for whom an initial course of antimony therapy had failed.

Methods.Forty subjects with clinical resistance to antimony were recruited in Lima, Peru, between February 2001 and December 2002. All subjects received meglumine antimoniate (20 mg/kg/day im or iv) and were randomized to receive either topical imiquimod 5% cream (Aldara; 3M Pharmaceuticals) or vehicle control every other day for 20 days. Lesions and adverse events were evaluated during treatment and at 1, 2, 3, 6, and 12 months after the treatment period.

Results.The mean number of lesions was 1.2 per person; 71% of the lesions were facial and 76% were ulcerative. There were no major differences between the groups, and all but 2 subjects completed therapy. Mild adverse events were reported by 73% of the subjects, but only erythema occurred more commonly in the imiquimod group ( ). Lesions resolved more rapidly in the imiquimod group: 50% of the imiquimod group achieved cure at 1 month after the treatment period versus 15% of the vehicle cream group ( ); 61% of the imiquimod group at 2 months versus 25% of the vehicle cream group ( ); and 72% of the imiquimod group at 3 months versus 35% of the vehicle cream group ( ). Residual scarring in the imiquimod group was less prominent than in the vehicle cream group.

Conclusions.Combined antimony plus imiquimod treatment was well tolerated, accelerated healing of lesions, and improved scar quality. This therapy may have particular advantages for subjects with facial lesions.

Received 10 September 2004; accepted 10 December 2004; electronically published 7 April 2005.

Reprints or correspondence: Dr. Brian Ward, McGill Centre for Tropical Diseases, McGill University Health Centre, Montreal, Canada 42810 ().

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  • Presented in part: 52nd Annual Meeting of the American Society of Tropical Medicine and Hygiene, Philadelphia, Pennsylvania, December 2003.

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