Novel agmatine analogue, g-guanidinooxypropylamine (GAPA) efficiently inhibits proliferation of Leishmania donovani by depletion of intracellular polyamine levels

Novel agmatine analogue, g-guanidinooxypropylamine (GAPA) efficiently inhibits proliferation of Leishmania donovani by depletion of intracellular polyamine levels

The efficacy of g-guanidinooxypropylamine (GAPA), a novel agmatine analogue against protozoan parasite, Leishmaniadonovani was evaluated. Wild-type and ornithine decarboxylase-overexpressors of L. donovani were used to study the effect and mode of action of this inhibitor. GAPA inhibited the growth...

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Bibliographic Details
Published in:Biochemical and biophysical research communications Vol. 375; no. 1; pp. 168 - 172
Main Authors: Singh, S, Jhingran, A, Sharma, A, Simonian, A R, Soininen, P, Vepsalainen, J, Khomutov, A R, Madhubala, R
Format: Journal Article
Language:English
Published: 10-10-2008
Subjects:
Leishmania donovani
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Summary:The efficacy of g-guanidinooxypropylamine (GAPA), a novel agmatine analogue against protozoan parasite, Leishmaniadonovani was evaluated. Wild-type and ornithine decarboxylase-overexpressors of L. donovani were used to study the effect and mode of action of this inhibitor. GAPA inhibited the growth of both promastigotes and amastigotes. Ornithine decarboxylase (ODC) activity and polyamine levels were markedly lower in cells treated with GAPA and proliferation was rescued by addition of putrescine or spermidine. GAPA inhibited L. donovani recombinant ODC with K sub(i) value of ~60kM. The ODC-overexpressors showed significant resistance to GAPA. GAPA has pK sub(a) 6.71 and at physiological pH the analogue can mimic protonated state of putrescine and can probably use putrescine transport system. Transport of putrescine in wild-type L. donovani promastigotes was inhibited by GAPA. We for the first time report that GAPA is a potential antileishmanial lead compound and it possibly inhibits L. donovani growth by depletion of intracellular polyamine levels.
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ISSN:0006-291X
DOI:10.1016/j.bbrc.2008.07.143