Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology

Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology

In Algeria, Leishmania infantum, Leishmania major, and Leishmania killicki (Leishmania tropica) are responsible for cutaneous leishmaniosis. We established a murine model of L. killicki infection to investigate its infective capacity, some immunophysiopathological aspects, and its suitability for ph...

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Main Authors: Naouel Eddaikra, Ihcene Kherachi Djenad, Sihem Benbetka, Razika Benikhlef, Khatima Aït-Oudhia, Farida Moulti-Mati, Bruno Oury, Denis Sereno, Zoubir Harrat
Format: Article
Language:English
Published: Hindawi Limited 2016-01-01
Series:BioMed Research International
Online Access:http://dx.doi.org/10.1155/2016/7985104
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spelling doaj-8d11c6994c5e4e068226b39a79a460ea2020-11-24T22:39:11ZengHindawi LimitedBioMed Research International2314-61332314-61412016-01-01201610.1155/2016/79851047985104Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in PharmacologyNaouel Eddaikra0Ihcene Kherachi Djenad1Sihem Benbetka2Razika Benikhlef3Khatima Aït-Oudhia4Farida Moulti-Mati5Bruno Oury6Denis Sereno7Zoubir Harrat8Laboratoire d’Eco-Épidemiologie Parasitaire et Génétique des Populations, Institut Pasteur d’Algerie, Route de Petit Staouéli, Dely Brahim, Algiers, AlgeriaLaboratoire d’Eco-Épidemiologie Parasitaire et Génétique des Populations, Institut Pasteur d’Algerie, Route de Petit Staouéli, Dely Brahim, Algiers, AlgeriaLaboratoire d’Eco-Épidemiologie Parasitaire et Génétique des Populations, Institut Pasteur d’Algerie, Route de Petit Staouéli, Dely Brahim, Algiers, AlgeriaLaboratoire d’Eco-Épidemiologie Parasitaire et Génétique des Populations, Institut Pasteur d’Algerie, Route de Petit Staouéli, Dely Brahim, Algiers, AlgeriaEcole Nationale Supérieure Vétérinaire, Hassan Badi, BP 161, El Harrach, Algiers, AlgeriaLaboratoire de Biochimie Analytique et Biotechnologies, Université Mouloud Mameri de Tizi-Ouzou, AlgeriaUnité Mixte de Recherche IRD 224 MiVegec (Maladies Infectieuses et Vecteurs: Écologie, Génétique, Évolution et Contrôle), Institut de Recherche pour le Développement (IRD), BP 64501, 34394 Montpellier Cedex 5, FranceUnité Mixte de Recherche IRD 224 MiVegec (Maladies Infectieuses et Vecteurs: Écologie, Génétique, Évolution et Contrôle), Institut de Recherche pour le Développement (IRD), BP 64501, 34394 Montpellier Cedex 5, FranceLaboratoire d’Eco-Épidemiologie Parasitaire et Génétique des Populations, Institut Pasteur d’Algerie, Route de Petit Staouéli, Dely Brahim, Algiers, AlgeriaIn Algeria, Leishmania infantum, Leishmania major, and Leishmania killicki (Leishmania tropica) are responsible for cutaneous leishmaniosis. We established a murine model of L. killicki infection to investigate its infective capacity, some immunophysiopathological aspects, and its suitability for pharmacological purposes. Following the injection of L. major or L. killicki metacyclic promastigotes in the ear dermis of BALB/c mice, the course of infection was followed. The infection with L. killicki caused slower lesion formation than with L. major. The presence of L. killicki or L. major DNA and parasites was detected in the ear dermis and in lymph nodes, spleen, and liver. Lesions induced by L. killicki were nonulcerative in their aspect, whereas those caused by L. major were highly ulcerative and necrotic, which matches well with the lesion phenotype reported in humans for L. killicki and L. major, respectively. The treatment of L. killicki lesions by injection of Glucantime® significantly reduced the lesion thickness and parasite burden. Ear dermal injection of BALB/c mice constitutes a model to study lesions physiopathology caused by L. killicki and presents interest for in vivo screening of new compounds against this pathogen, emerging in Algeria.http://dx.doi.org/10.1155/2016/7985104
collection DOAJ
language English
format Article
sources DOAJ
author Naouel Eddaikra
Ihcene Kherachi Djenad
Sihem Benbetka
Razika Benikhlef
Khatima Aït-Oudhia
Farida Moulti-Mati
Bruno Oury
Denis Sereno
Zoubir Harrat
spellingShingle Naouel Eddaikra
Ihcene Kherachi Djenad
Sihem Benbetka
Razika Benikhlef
Khatima Aït-Oudhia
Farida Moulti-Mati
Bruno Oury
Denis Sereno
Zoubir Harrat
Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology
BioMed Research International
author_facet Naouel Eddaikra
Ihcene Kherachi Djenad
Sihem Benbetka
Razika Benikhlef
Khatima Aït-Oudhia
Farida Moulti-Mati
Bruno Oury
Denis Sereno
Zoubir Harrat
author_sort Naouel Eddaikra
title Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology
title_short Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology
title_full Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology
title_fullStr Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology
title_full_unstemmed Development of a Murine Infection Model with Leishmania killicki, Responsible for Cutaneous Leishmaniosis in Algeria: Application in Pharmacology
title_sort development of a murine infection model with leishmania killicki, responsible for cutaneous leishmaniosis in algeria: application in pharmacology
publisher Hindawi Limited
series BioMed Research International
issn 2314-6133
2314-6141
publishDate 2016-01-01
description In Algeria, Leishmania infantum, Leishmania major, and Leishmania killicki (Leishmania tropica) are responsible for cutaneous leishmaniosis. We established a murine model of L. killicki infection to investigate its infective capacity, some immunophysiopathological aspects, and its suitability for pharmacological purposes. Following the injection of L. major or L. killicki metacyclic promastigotes in the ear dermis of BALB/c mice, the course of infection was followed. The infection with L. killicki caused slower lesion formation than with L. major. The presence of L. killicki or L. major DNA and parasites was detected in the ear dermis and in lymph nodes, spleen, and liver. Lesions induced by L. killicki were nonulcerative in their aspect, whereas those caused by L. major were highly ulcerative and necrotic, which matches well with the lesion phenotype reported in humans for L. killicki and L. major, respectively. The treatment of L. killicki lesions by injection of Glucantime® significantly reduced the lesion thickness and parasite burden. Ear dermal injection of BALB/c mice constitutes a model to study lesions physiopathology caused by L. killicki and presents interest for in vivo screening of new compounds against this pathogen, emerging in Algeria.
url http://dx.doi.org/10.1155/2016/7985104
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