Title of article
Synthesis and antileishmanial activity of novel buparvaquone oxime derivatives Original Research Article
Author/Authors
Antti M?ntyl?، نويسنده , , Jarkko Rautio، نويسنده , , Tapio Nevalainen، نويسنده , , Jouko Veps?lainen، نويسنده , , Risto Juvonen، نويسنده , , Howard Kendrick، نويسنده , , Tracy Garnier، نويسنده , , Simon L. Croft، نويسنده , , Tomi Jarvinen، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2004
Pages
6
From page
3497
To page
3502
Abstract
Novel oxime derivatives (2, 3 and 5) of buparvaquone (1) and O-methyl-buparvaquone (4) were synthesized and their in vitro activities against Leishmania donovani, the causative agent of visceral leishmaniasis (VL), were determined. Buparvaquone-oxime (2) was also studied as a bioreversible prodrug structure of buparvaquone (1). Buparvaquone-oxime (2) released buparvaquone (1) in vitro when it was incubated with induced rat liver microsomes, which suggests that the oxime-structure is a useful prodrug template for developing novel prodrugs of buparvaquone and other hydroxynaphthoquinones. Moreover, the formation of NO2−, formed via oxidation of NO, was confirmed during the bioconversion. The release of NO from buparvaquone-oxime (2) may provide an additional therapeutic effect in the treatment of leishmaniasis. Buparvaquone-oxime (2) and buparvaquone-O-methyloxime (3) demonstrated moderate activity against amastigotes of the Leishmania species that causes VL. However, the studied oximes (2, 3) most probably did not release buparvaquone (1) and NO during the present in vitro experiment. Further in vivo studies are needed to verify the biological activity of buparvaquone-oximes in the treatment of leishmaniasis.
Keywords
leishmaniasis , nitric oxide , Oxime , Buparvaquone , Prodrug
Journal title
Bioorganic and Medicinal Chemistry
Serial Year
2004
Journal title
Bioorganic and Medicinal Chemistry
Record number
1303150
Link To Document