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Cysteine protease inhibitors as chemotherapy: Lessons from a parasite target

Authors :
James H. McKerrow
Bernhard Ugele
Ivy Hsieh
David G. Russell
Victor J. Chan
Judy A. Sakanari
Paul M. Selzer
Juan C. Engel
Sabine Pingel
Matthew Bogyo
Source :
ResearcherID
Publication Year :
1999
Publisher :
The National Academy of Sciences, 1999.

Abstract

Papain family cysteine proteases are key factors in the pathogenesis of cancer invasion, arthritis, osteoporosis, and microbial infections. Targeting this enzyme family is therefore one strategy in the development of new chemotherapy for a number of diseases. Little is known, however, about the efficacy, selectivity, and safety of cysteine protease inhibitors in cell culture orin vivo. We now report that specific cysteine protease inhibitors killLeishmaniaparasitesin vitro, at concentrations that do not overtly affect mammalian host cells. Inhibition ofLeishmaniacysteine protease activity was accompanied by defects in the parasite’s lysosome/endosome compartment resembling those seen in lysosomal storage diseases. Colocalization of anti-protease antibodies with biotinylated surface proteins and accumulation of undigested debris and protease in the flagellar pocket of treated parasites were consistent with a pathway of protease trafficking from flagellar pocket to the lysosome/endosome compartment. The inhibitors were sufficiently absorbed and stablein vivoto ameliorate the pathology associated with a mouse model ofLeishmaniainfection.

Details

Language :
English
Database :
OpenAIRE
Journal :
ResearcherID
Accession number :
edsair.doi.dedup.....da7e549e6cc5c39be725ed270c976145