Prevention of HIV-1 infection and preservation of CD4 function by the binding of CPFs to gp120.

Science
Authors
Keywords
Abstract

Infection by human immunodeficiency virus type-1 (HIV-1) is initiated when its envelope protein, gp120, binds to its receptor, the cell surface glycoprotein CD4. Small molecules, termed N-carbomethoxycarbonyl-prolyl-phenylalanyl benzyl esters (CPFs), blocked this binding. CPFs interacted with gp120 and did not interfere with the binding of CD4 to class II major histocompatibility complex molecules. One CPF isomer, CPF(DD), preserved CD4-dependent T cell function while inhibiting HIV-1 infection of H9 tumor cells and human T cells. Although the production of viral proteins in infected T cells is unaltered by CPF(DD), this compound prevents the spread of infection in an in vitro model system.

Year of Publication
1990
Journal
Science
Volume
249
Issue
4966
Pages
287-91
Date Published
1990 Jul 20
ISSN
0036-8075
PubMed ID
2115689
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