Literature DB >> 8913444

In vivo efficacy of oral and intralesional administration of 2-substituted quinolines in experimental treatment of new world cutaneous leishmaniasis caused by Leishmania amazonensis.

A Fournet1, M E Ferreira, A Rojas De Arias, S Torres De Ortiz, S Fuentes, H Nakayama, A Schinini, R Hocquemiller.   

Abstract

The antileishmanial efficacies of 2-n-propylquinoline, chimanines B and D, 2-n-pentylquinoline, 2-phenylquinoline, 2-(3,4-methylenedioxyphenylethyl) quinoline, and two total alkaloidal extracts of Galipea longiflora were evaluated in BALB/c mice infected with Leishmania amazonensis or Leishmania venezuelensis. Animals were treated for 4 to 6 weeks postinfection with a quinoline by the oral route at 50 mg/kg of body weight twice daily for 15 days or by five intralesional injections at intervals of 4 days with a quinoline at 50 mg/kg of body weight. The reference drug, N-methylglucamine antimonate (Glucantime), was administered by subcutaneous or intralesional injection (regimens of 14, 28, or 56 mg of pentavalent antimony [Sbv] per kg of body weight daily). Twice-daily oral treatment with chimanine B at 50 mg/kg resulted in a decrease in lesion weight by 70% (P < 0.001) and a decrease in the parasite loads by 95% (P < 0.001). Five injections of chimanine B at intervals of 4 days reduced the lesion weight by 74% and the parasite loads in the lesion by 90% compared with the values for the group of untreated mice. Subcutaneous administration of N-methylglucamine antimonate at 28 mg of Sbv kg per day for 15 days reduced the parasite burden by 95% (P < 0.001), and five intralesional injections at the same concentration reduced the parasite burden by 96% (P < 0.001). Other 2-substituted quinolines, 2-n-propylquinoline administered by the oral and intralesional routes, 2-phenylquinoline administered by the oral route, 2-n-pentylquinoline administered by intralesional injection, and two total alkaloidal extracts of G. longiflora administered by the oral route, had intermediate effects. These findings suggest that chimanine B may be chosen as a lead molecule in the development of oral therapy against leishmaniasis.

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Year:  1996        PMID: 8913444      PMCID: PMC163555     

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  16 in total

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3.  The activity of 2-substituted quinoline alkaloids in BALB/c mice infected with Leishmania donovani.

Authors:  A Fournet; J C Gantier; A Gautheret; L Leysalles; M H Munos; J Mayrargue; H Moskowitz; A Cavé; R Hocquemiller
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4.  2-substituted quinoline alkaloids as potential antileishmanial drugs.

Authors:  A Fournet; A A Barrios; V Muñoz; R Hocquemiller; A Cavé; J Bruneton
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5.  Medicinal plants in the fight against leishmaniasis.

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6.  Treatment of atypical leishmaniasis with interferon gamma resulting in progression of Kaposi's sarcoma in an AIDS patient.

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7.  Drug resistance in leishmaniasis: its implication in systemic chemotherapy of cutaneous and mucocutaneous disease.

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8.  Up-regulation of T helper 2 and down-regulation of T helper 1 cytokines during murine retrovirus-induced immunodeficiency syndrome enhances susceptibility of a resistant mouse strain to Leishmania amazonensis.

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9.  Immune responses associated with susceptibility of C57BL/10 mice to Leishmania amazonensis.

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  19 in total

1.  Efficacy of orally administered 2-substituted quinolines in experimental murine cutaneous and visceral leishmaniases.

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2.  Synthesis and antileishmanial activities of novel 3-substituted quinolines.

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6.  Microwave-assisted, rapid synthesis of 2-vinylquinolines and evaluation of their antimalarial activity.

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8.  Antileishmanial activity of a formulation of 2-n-propylquinoline by oral route in mice model.

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Review 9.  The Potential of Traditional Knowledge to Develop Effective Medicines for the Treatment of Leishmaniasis.

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