Bulletin of Experimental Treatments for AIDS, No. 26 September 1995
Ronald Baker, PhD

Hydroxyurea does not act directly against HIV, but rather depletes cells of deoxynucleoside triphosphates (dNTP), which are crucial components (building blocks) of DNA synthesis. "When HIV enters a cell depleted of dNTP by the action of hydroxyurea, there is not enough of the building blocks present for the virus to survive," explains Franco Lori, MD, of the research Institute for Genetic and Human Therapy in Pavia, Italy. In combination with ddI, Lori says, hydroxyurea decreases viral replication so dramatically that there's less virus available to mutate, possibly delaying the onset of resistance to ddI.

"Hydroxyurea may permit a significant reduction in the toxicity of ddI, since we would like to combine the 2 drugs at low doses," says Lawrence Fox, MD, of the National Institute of Allergy and Infectious Diseases (NIAID). Fox says he is skeptical about hydroxyurea in combination with AZT because both agents cause bone marrow toxicity. A controlled, triple combination study of hydroxyurea plus ddI plus d4T is scheduled to start in August, sponsored by the Shared Medical Research Foundation of Tarzana, California. See also page 71 of the March 1995 issue of BETA.

950901
BETA2611

Copyright © 1995 - Bulletin of Experimental Treatments for AIDS (BETA). Reproduced with permission. BETA is published four times a year by the San Francisco AIDS Foundation. All rights reserved. Noncommercial reproduction is encouraged. Subscription lists are kept confidential. Call 415.487.8060; FAX: 415.487.8069. Mailing Address: P.O. Box 426182, San Francisco, CA 94142-6182.  beta@sfaf.org  http://www.sfaf.org/beta.html