Nitric Oxide-Mediated Proteasome-Dependent Oligonucleosomal DNA Fragmentation in Leishmania amazonensis Amastigotes

doi:10.1128/IAI.70.7.3727-3735.2002

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Infection and Immunity, July 2002, p. 3727-3735, Vol. 70, No. 7
0019-9567/02/$04.00+0 DOI: 10.1128/IAI.70.7.3727-3735.2002
Copyright © 2002, American Society for Microbiology. All Rights Reserved.

Nitric Oxide-Mediated Proteasome-Dependent Oligonucleosomal DNA Fragmentation in Leishmania amazonensis Amastigotes

Philippe Holzmuller,¹ Denis Sereno,¹ Mireille Cavaleyra,¹ Isabelle Mangot,¹ Sylvie Daulouede,² Philippe Vincendeau,² and Jean-Loup Lemesre¹^*

UR 008 Pathogénie des Trypanosomatidés, Institut de Recherche pour le Développement, 34032 Montpellier Cedex 1,¹ Laboratoire de Parasitologie, Université Victor Segalen Bordeaux II, 33076 Bordeaux Cedex, France²

Received 4 September 2001/ Returned for modification 15 November 2001/ Accepted 21 March 2002

Resistance to leishmanial infections depends on intracellularparasite killing by activated host macrophages through the L-arginine-nitricoxide (NO) metabolic pathway. Here we investigate the cell deathprocess induced by NO for the intracellular protozoan Leishmaniaamazonensis. Exposure of amastigotes to moderate concentrationsof NO-donating compounds (acidified sodium nitrite NaNO₂ ornitrosylated albumin) or to endogenous NO produced by lipopolysaccharideor gamma interferon treatment of infected macrophages resultedin a dramatic time-dependent cell death. The combined use ofseveral standard DNA status analysis techniques (including electrophoresisladder banding patterns, YOPRO-1 staining in flow cytofluorometry,and in situ recognition of DNA strand breaks by TUNEL [terminaldeoxynucleotidyltransferase-mediated dUTP-biotin nick end labeling]assay) revealed a rapid and extensive fragmentation of nuclearDNA in both axenic and intracellular NO-treated amastigotesof L. amazonensis. Despite some similarities to apoptosis, thenuclease activation responsible for characteristic DNA degradationwas not under the control of caspase activity as indicated bythe lack of involvement of cell-permeable inhibitors of caspasesand cysteine proteases. In contrast, exposure of NO-treatedamastigotes with specific proteasome inhibitors, such as lactacystinor calpain inhibitor I, markedly reduced the induction of theNO-mediated apoptosis-like process. These data strongly suggestthat NO-induced oligonucleosomal DNA fragmentation in Leishmaniaamastigotes is, at least in part, regulated by noncaspase proteasesof the proteasome. The determination of biochemical pathwaysleading up to cell death might ultimately allow the identificationof new therapeutic targets.

* Corresponding author. Mailing address: UR 008 Pathogénie des Trypanosomatidés, IRD (Institut de Recherche pour le Développement), 911 Ave. Agropolis, BP 5045, 34032 Montpellier Cedex 1, France. Fax: 33(0)4-67-41-63-30. Phone: 33(0)4-67-41-62-20. E-mail: lemesre{at}melusine.mpl.ird.fr.

Editor: B. B. Finlay

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