Dynamics of immune granuloma formation in a Leishmania braziliensis-induced self-limiting cutaneous infection in the primate Macaca mulatta

In order to unravel the physiopathology of leishmaniasis in humans, it is necessary to better understand how Leismania are able to survive for years within immunologically active granulomas. In the present study, we used a macaque (Macaca mulatta) model of infection with Leishmania braziliensis as a...

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Published in:	The Journal of pathology Vol. 216; no. 3; pp. 375 - 386
Main Authors:	Souza-Lemos, C, de-Campos, SN, Teva, A, Côrte-Real, S, Fonseca, EC, Porrozzi, R, Grimaldi, G. Jr
Format:	Journal Article
Language:	English
Published:	Chichester, UK John Wiley & Sons, Ltd 01-11-2008
Subjects:	Animals Antigens, Protozoan - analysis Chemotaxis, Leukocyte cutaneous infection Flow Cytometry Granuloma - immunology Granuloma - parasitology human-like granulomatous response Immunophenotyping Leishmania braziliensis Leishmania braziliensis - physiology Leishmania braziliensis - ultrastructure Leishmaniasis, Cutaneous - immunology Leukocyte Count Macaca mulatta - immunology Macaca mulatta - parasitology Male Microscopy, Electron Models, Animal Monkey Diseases - immunology Monkey Diseases - parasitology primate model Skin - immunology Skin - parasitology T-Lymphocytes - immunology
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Summary:	In order to unravel the physiopathology of leishmaniasis in humans, it is necessary to better understand how Leismania are able to survive for years within immunologically active granulomas. In the present study, we used a macaque (Macaca mulatta) model of infection with Leishmania braziliensis as a means of assessing the usefulness of this primate system. This model more closely mirrors human protective immunity to Leishmania than the murine model; therefore, we used it to study the host inflammatory granulomatous response involved in the control of cutaneous leishmaniasis. Infected primates developed localized long-term skin ulcerations, but complete spontaneous clinical healing occurred in all infected animals. The infection induced the recruitment and activation of inflammatory mast cells, granulocytes, mononuclear phagocytes, and lymphocytes at the site of infection. During the acute reaction, polymorphonuclear leukocytes were more prominent than other cell types and apparently destroyed many parasites; macrophages then rapidly engulfed dying neutrophils together with their parasitic cargo. In the chronic phase, persisting parasites induced a typical T helper (Th) cytokine, type 1-mediated, immunity-induced granulomatous reaction. By this time, more or less differentiated macrophage accumulations were found, and these evolved to become mature tissue granulomas consisting of all the specific cell types found within human granulomas. In the healing stage, fibroblasts proliferated at the periphery and finally invaded the granulomas with fibrotic substitution. These findings point to the feasibility of using this model to elucidate the potentially disabling Th1-cell mechanisms that may eventually render the host granulomatous response inadequate for fighting L. braziliensis infections. Copyright © 2008 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.
Bibliography:	http://dx.doi.org/10.1002/path.2403 Millennium Institute for Vaccine Development and Technology - No. MCT/CNPq-420067/2005-1 Fiocruz, Edital - No. MCT/CNPq-470269/2006-5 ArticleID:PATH2403 istex:43326E6B3702D4AE0BB38B5ADB6CCDD92499E266 ark:/67375/WNG-M7SR96KG-7 The authors have no conflicts of interest concerning the work reported in this article. ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23
ISSN:	0022-3417 1096-9896
DOI:	10.1002/path.2403