The multifactorial nature of HIV-1 latency

Kara Lassen; Yefei Han; Yan Zhou; Janet Siliciano; Robert F. Siliciano

doi:10.1016/j.molmed.2004.09.006

The multifactorial nature of HIV-1 latency

Kara Lassen, Yefei Han, Yan Zhou, Janet Siliciano, Robert F. Siliciano

School of Medicine

Research output: Contribution to journal › Review article › peer-review

199 Scopus citations

Abstract

HIV-1 can avoid host immune responses and antiretroviral drugs through the latent infection of resting memory CD4 ⁺ T cells. Recently, latent viral genomes have been shown to reside within the introns of active host genes. Therefore, latency is not simply due to an inaccessibility of the integrated proviruses to the transcriptional machinery. Rather, latency might result from insufficient nuclear levels of the crucial activation-dependent host transcription factors required to overcome the transcriptional interference that is an automatic consequence of the nature of HIV-1 integration sites. In addition, resting cells lack sufficient levels of HIV-1 Tat and Tat-associated activation-dependent host factors that are necessary for processive transcription. Defects at consecutive steps of transcriptional initiation and elongation enable HIV-1 to remain hidden within resting CD4 ⁺ T cells.

Original language	English (US)
Pages (from-to)	525-531
Number of pages	7
Journal	Trends in Molecular Medicine
Volume	10
Issue number	11
DOIs	https://doi.org/10.1016/j.molmed.2004.09.006
State	Published - Nov 2004

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology

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10.1016/j.molmed.2004.09.006

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title = "The multifactorial nature of HIV-1 latency",

abstract = "HIV-1 can avoid host immune responses and antiretroviral drugs through the latent infection of resting memory CD4 + T cells. Recently, latent viral genomes have been shown to reside within the introns of active host genes. Therefore, latency is not simply due to an inaccessibility of the integrated proviruses to the transcriptional machinery. Rather, latency might result from insufficient nuclear levels of the crucial activation-dependent host transcription factors required to overcome the transcriptional interference that is an automatic consequence of the nature of HIV-1 integration sites. In addition, resting cells lack sufficient levels of HIV-1 Tat and Tat-associated activation-dependent host factors that are necessary for processive transcription. Defects at consecutive steps of transcriptional initiation and elongation enable HIV-1 to remain hidden within resting CD4 + T cells.",

author = "Kara Lassen and Yefei Han and Yan Zhou and Janet Siliciano and Siliciano, {Robert F.}",

note = "Funding Information: This work was supported by NIH grant AI43222 and by the Doris Duke Charitable Foundation and the Howard Hughes Medical Institute.",

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AU - Lassen, Kara

AU - Han, Yefei

AU - Zhou, Yan

AU - Siliciano, Janet

AU - Siliciano, Robert F.

N1 - Funding Information: This work was supported by NIH grant AI43222 and by the Doris Duke Charitable Foundation and the Howard Hughes Medical Institute.

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N2 - HIV-1 can avoid host immune responses and antiretroviral drugs through the latent infection of resting memory CD4 + T cells. Recently, latent viral genomes have been shown to reside within the introns of active host genes. Therefore, latency is not simply due to an inaccessibility of the integrated proviruses to the transcriptional machinery. Rather, latency might result from insufficient nuclear levels of the crucial activation-dependent host transcription factors required to overcome the transcriptional interference that is an automatic consequence of the nature of HIV-1 integration sites. In addition, resting cells lack sufficient levels of HIV-1 Tat and Tat-associated activation-dependent host factors that are necessary for processive transcription. Defects at consecutive steps of transcriptional initiation and elongation enable HIV-1 to remain hidden within resting CD4 + T cells.

AB - HIV-1 can avoid host immune responses and antiretroviral drugs through the latent infection of resting memory CD4 + T cells. Recently, latent viral genomes have been shown to reside within the introns of active host genes. Therefore, latency is not simply due to an inaccessibility of the integrated proviruses to the transcriptional machinery. Rather, latency might result from insufficient nuclear levels of the crucial activation-dependent host transcription factors required to overcome the transcriptional interference that is an automatic consequence of the nature of HIV-1 integration sites. In addition, resting cells lack sufficient levels of HIV-1 Tat and Tat-associated activation-dependent host factors that are necessary for processive transcription. Defects at consecutive steps of transcriptional initiation and elongation enable HIV-1 to remain hidden within resting CD4 + T cells.

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The multifactorial nature of HIV-1 latency

Abstract

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