A Tat antagonist inhibits HIV-1 induction in naturally infected and experimentally infected T cells

Mary Jane Potash; Galina Bentsman; George McKinley; David J. Volsky

doi:10.1016/0006-291X(92)91551-Z

A Tat antagonist inhibits HIV-1 induction in naturally infected and experimentally infected T cells

Mary Jane Potash, Galina Bentsman, George McKinley, David J. Volsky

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Ro 5-3335, a novel antagonist of human immunodeficiency virus type 1 (HIV-1) Tat activity, inhibits acute and chronic HIV-1 infection in T lymphocytes. Here we describe the effects of Ro 5-3335 on the accumulation of viral DNA during primary infection, the induction of virus from a latently infected cell line, and the expression of virus upon activation of naturally infected T cells. Ro 5-3335 permitted initial DNA synthesis during primary infection, but inhibited the subsequent increase in viral DNA copy number. The induction of HIV-1, as determined by the synthesis of p24 core antigen, was inhibited by 99% by Ro 5-3335 in both the model cell line and naturally infected T cells.

Original language	English
Pages (from-to)	250-256
Number of pages	7
Journal	Biochemical and Biophysical Research Communications
Volume	189
Issue number	1
DOIs	https://doi.org/10.1016/0006-291X(92)91551-Z
State	Published - 30 Nov 1992

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title = "A Tat antagonist inhibits HIV-1 induction in naturally infected and experimentally infected T cells",

abstract = "Ro 5-3335, a novel antagonist of human immunodeficiency virus type 1 (HIV-1) Tat activity, inhibits acute and chronic HIV-1 infection in T lymphocytes. Here we describe the effects of Ro 5-3335 on the accumulation of viral DNA during primary infection, the induction of virus from a latently infected cell line, and the expression of virus upon activation of naturally infected T cells. Ro 5-3335 permitted initial DNA synthesis during primary infection, but inhibited the subsequent increase in viral DNA copy number. The induction of HIV-1, as determined by the synthesis of p24 core antigen, was inhibited by 99% by Ro 5-3335 in both the model cell line and naturally infected T cells.",

author = "Potash, {Mary Jane} and Galina Bentsman and George McKinley and Volsky, {David J.}",

note = "Funding Information: ACKNOWLEDGMENTS We thank M. G. Pellegrino for expert technical M.-C. Hsu for the generous gift of Ro 5-3335. supported by PHS Awards AI 27397 and AI 25902.",

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T1 - A Tat antagonist inhibits HIV-1 induction in naturally infected and experimentally infected T cells

AU - Potash, Mary Jane

AU - Bentsman, Galina

AU - McKinley, George

AU - Volsky, David J.

N1 - Funding Information: ACKNOWLEDGMENTS We thank M. G. Pellegrino for expert technical M.-C. Hsu for the generous gift of Ro 5-3335. supported by PHS Awards AI 27397 and AI 25902.

PY - 1992/11/30

Y1 - 1992/11/30

N2 - Ro 5-3335, a novel antagonist of human immunodeficiency virus type 1 (HIV-1) Tat activity, inhibits acute and chronic HIV-1 infection in T lymphocytes. Here we describe the effects of Ro 5-3335 on the accumulation of viral DNA during primary infection, the induction of virus from a latently infected cell line, and the expression of virus upon activation of naturally infected T cells. Ro 5-3335 permitted initial DNA synthesis during primary infection, but inhibited the subsequent increase in viral DNA copy number. The induction of HIV-1, as determined by the synthesis of p24 core antigen, was inhibited by 99% by Ro 5-3335 in both the model cell line and naturally infected T cells.

AB - Ro 5-3335, a novel antagonist of human immunodeficiency virus type 1 (HIV-1) Tat activity, inhibits acute and chronic HIV-1 infection in T lymphocytes. Here we describe the effects of Ro 5-3335 on the accumulation of viral DNA during primary infection, the induction of virus from a latently infected cell line, and the expression of virus upon activation of naturally infected T cells. Ro 5-3335 permitted initial DNA synthesis during primary infection, but inhibited the subsequent increase in viral DNA copy number. The induction of HIV-1, as determined by the synthesis of p24 core antigen, was inhibited by 99% by Ro 5-3335 in both the model cell line and naturally infected T cells.

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A Tat antagonist inhibits HIV-1 induction in naturally infected and experimentally infected T cells

Abstract

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