In VivoAntiviral Activity of Novel Human Immunodeficiency Virus Type 1 Nucleocapsid p7 Zinc Finger Inhibitors in a Transgenic Murine Model

Schito, Marco L. ; Goel, Atul ; Song, Yongsheng ; Inman, John K. ; Fattah, Rasem J. ; Rice, William G. ; Turpin, Jim A. ; Sher, Alan ; Appella, Ettore (2003) In VivoAntiviral Activity of Novel Human Immunodeficiency Virus Type 1 Nucleocapsid p7 Zinc Finger Inhibitors in a Transgenic Murine Model AIDS Research and Human Retroviruses, 19 (2). pp. 91-101. ISSN 0889-2229

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Official URL: http://doi.org/10.1089/088922203762688595

Related URL: http://dx.doi.org/10.1089/088922203762688595

Abstract

Control of human immunodeficiency virus through the use of inexpensive chemotherapeutics, with minimal side effects and decreased potential for engendering resistant virus, is a long-term therapeutic goal. In principle, this goal can be accomplished if viral replication in reservoirs of chronically and latently infected cells is addressed. As a first step, we have developed novel antiviral compounds based on a 2-mercaptobenzamide thioester chemotype, including the pyridinioalkanoyl thioesters, which specifically target the zinc fingers of the human immunodeficiency virus nucleocapsid protein (NCp7). Using these compounds in a murine transgenic model, in which infectious human immunodeficiency virus is induced from an integrated provirus, we show inhibition of transgenic spleen cell p24 expression with potencies comparable to acute infection assays using human peripheral blood lymphocytes. More importantly, transgenic mice treated in vivo with two 2-mercaptobenzamide thioesters expressed significantly lower plasma p24, and splenocytes from these animals produced fewer infectious virions. Thus, these thioesters may provide an effective means for inhibiting the expression of human immunodeficiency virus from integrated viral reservoirs.

Item Type:Article
Source:Copyright of this article belongs to Mary Ann Liebert, Inc.
ID Code:117899
Deposited On:06 May 2021 06:24
Last Modified:06 May 2021 06:24

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