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Preclinical Development of HIV-1 Vif Antagonists

$1,326,345U19FY2008MHNIH

Univ Of Massachusetts Med Sch Worcester, Worcester MA

Investigators

Linked publications & trials

Abstract

PROVIDED.[unreadable] This application proposes the identification and preclinical development of novel small molecule antagonists[unreadable] of the Vif protein of HIV-1. Apobec 3G is a cytidine deaminase which potently antagonizes HIV-1 infection.[unreadable] To counteract this cellular restriction, primate lentiviruses such as HIV-1 have evolved a Vif protein, the[unreadable] function of which is to target apobec for proteasomal destruction. Viruses containing mutations in Vif are[unreadable] severely compromised in vitro and in vivo. Therefore, Vif is a critical, yet unrealized, therapeutic target.[unreadable] Through institutional support and a grant from Howard Hughes Medical Institute, UMass Medical School[unreadable] (UMMS) has recently established a high throughput inhibitor screening facility and the identification of[unreadable] compounds that block the action of HIV-1 Vif was prioritized. As a result of this initial screening, two lead[unreadable] compounds that block Vif-mediated apobec destruction have been identified. These compounds inhibit HIV-[unreadable] 1 replication only in the presence of apobec and as such, are bona fide Vif inhibitors. This provides proof-ofprinciple[unreadable] that novel inhibitors of the HIV-1 Vif protein can be identified. This program project application will[unreadable] combine individuals with expertise in drug discovery, HIV-1 virology and SIV immunopathogenesis for the[unreadable] preclinical development of novel antagonists of HIV-1 Vif. The program project comprises:[unreadable] Project 1, T. Rana, Ph.D., UMMS, Vif antagonists: lead inhibitor identification and SAR analysis.[unreadable] Project 2, M. Stevenson, Ph.D., UMMS, Vif antagonists: evaluation of antiviral activity and[unreadable] mechanism of action in vitro. Mechanisms of inhibitor resistance in vitro and in vivo.[unreadable] Project 3, K. Mansfield, D.V.M., Harvard and NEPRC, Vif-antagonists: small animal PK and toxicity[unreadable] profiling, evaluation in chronic SIV infection model and in model of SIV-induced encephalitis.[unreadable] Core A, Administrative Core[unreadable] Core B, B. Beer, Ph.D., Southern Research Institute, Vif-antagonists: inhibitor sensitivity of clinical[unreadable] HIV-1 isolates, and plasma SIV RNA assays in treated monkeys.[unreadable] Through this program project, we propose the preclinical development of a new class of compounds that[unreadable] antagonize HIV-1 and SIV Vif and which will be used to assess the consequences of Vif antagonism in[unreadable] lymphoid and CNS reservoirs of viral replication in vivo.

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