Activities of dl -α-Difluoromethylarginine and Polyamine Analogues against Cryptosporidium parvum Infection in a T-Cell Receptor Alpha-Deficient Mouse Model

Author:

Yarlett Nigel12,Waters W. Ray3,Harp James A.3,Wannemuehler Michael J.4,Morada Mary1,Bellcastro Josephine1,Upton Steve J.5,Marton Laurence J.6,Frydman Benjamin J.7

Affiliation:

1. Haskins Laboratories

2. Department of Chemistry and Physical Sciences, Pace University, New York, New York 10038

3. National Animal Disease Center, Agricultural Research Service, U.S. Department of Agriculture, Ames, Iowa 50010

4. Veterinary Medical Research Institute, Iowa State University, Ames, Iowa 50011

5. Kansas State University, Manhattan, Kansas 66506

6. Cellgate, Redwood City, California 94065

7. Omnisynthesis LLC, Madison, Wisconsin 53711

Abstract

ABSTRACT The in vivo effectiveness of a series of conformationally restricted polyamine analogues alone and selected members in combination with dl -α-difluoromethylarginine against Cryptosporidium parvum infection in a T-cell receptor alpha-deficient mouse model was tested. Polyamine analogues were selected from the extended bis(ethyl)- sym -homospermidine or bis(ethyl)-spermine backbone having cis or trans double bonds at the center of the molecule. The cis isomers were found to have significantly greater efficacy in both preventing and curing infection in a mouse model than the trans polyamine analogues when tested in a T-cell receptor alpha-deficient mouse model. When tested in combination with dl -α-difluoromethylarginine, the cis -restricted analogues were found to be more effective in preventing oocyst shedding. This study demonstrates the potential of polyamine analogues as anticryptosporidial agents and highlights the presence of multiple points in polyamine synthesis by this parasite that are susceptible to inhibition resulting in growth inhibition.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology

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