1. Dynamics of Parasite Clearance in Cutaneous Leishmaniasis Patients Treated with Miltefosine.
- Author
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Dorlo, Thomas P. C., van Thiel, Pieter P. A. M., Schoone, Gerard J., Stienstra, Ymkje, van Vugt, Michèle, Beijnen, Jos H., and de Vries, Peter J.
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CUTANEOUS leishmaniasis ,MILTEFOSINE ,DRUG efficacy ,CLINICAL trials ,LEISHMANIA major ,LEISHMANIA mexicana - Abstract
Parasite loads were quantified in repeated skin biopsies from lesions of 2 patients with Old-World cutaneous leishmaniasis (CL) caused by Leishmania major and L. infantum during and after treatment with miltefosine. Miltefosine induced a rapid therapeutic effect on both infections with an initial decline of parasites of ∼1 log/week for the L. major infection. These observations illustrate the usability of quantifying parasite loads in skin lesions as a pharmacodynamic measure and quantitative descriptor of drug effect for CL supporting clinical assessment. Author Summary: The clinical evaluation of the ulcerated lesions in cutaneous leishmaniasis (CL) is both difficult and subjective. As a result, the evaluation of therapeutic efficacy of drugs for CL remains complicated. The relationship between dose and effect of antileishmanial drugs in CL is unclear and a good quantitative descriptor of drug effect has not yet been established. This report describes the use of quantifying the parasite load in repeated full-thickness skin biopsies from lesions of two patients with extensive Old-World CL (Leishmania major and L. infantum) who both were treated with miltefosine to demonstrate the dynamics of parasite clearance within CL lesions. Therapeutic effect of miltefosine was already noticeable directly after start of treatment, with a rapid, log-linear decline in parasite load in the skin biopsies of approximately 1 log/week for the L. major infection. These observations illustrate the applicability of quantifying parasite loads as a pharmacodynamic measure for CL supporting clinical assessment. The methodology described here might enable better evaluation and comparison of standard and new therapeutics in future randomized clinical trials for CL. [ABSTRACT FROM AUTHOR]
- Published
- 2011
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