Macrophage-directed delivery of doxorubicin conjugated to neoglycoprotein using leishmaniasis as the model disease

Sett, Rupnarayan ; Sarkar, Kakali ; Das, Pijush K. (1993) Macrophage-directed delivery of doxorubicin conjugated to neoglycoprotein using leishmaniasis as the model disease Journal of Infectious Diseases, 168 (4). pp. 994-999. ISSN 0022-1899

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Official URL: http://jid.oxfordjournals.org/content/168/4/994.ab...

Related URL: http://dx.doi.org/10.1093/infdis/168.4.994

Abstract

The antileishmanial potency of doxorubicin conjugated to mannose-human serum albumin (man-HSA) was tested in experimental visceral leishmaniasis. Conjugation of doxorubicin did not decrease the affinity of the neoglycoprotein for the macrophage mannose receptor. Conjugated doxorubicin eliminated intracellular amastigotes of Leishmania donovani in peritoneal macrophages almost 12.5 times more efficiently than did the free drug and greatly reduced and possibly eliminated splenic intracellular parasites in four consecutive dosages at 5 µg/kg/day for 45 days. Free drug at a similar dose had little effect. The leishmanicidal effect of doxorubicin conjugate can be prevented by competitive inhibitors such as man-HSA or mannan and inhibitors of receptor-mediated endocytosis such as colchicine and monensin. These results not only indicate the potential ofdoxorubicin as an effective chemotherapeutic agent for leishmaniasis but also establish the use of mannosylated neoglycoprotein as a drug carrier in the therapy of macrophage- associated diseases.

Item Type:Article
Source:Copyright of this article belongs to University of Chicago Press.
ID Code:93786
Deposited On:27 Jun 2012 11:06
Last Modified:27 Jun 2012 11:06

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