Tat is required for efficient HIV-1 reverse transcription

Harrich, David; Ulich, Catherine; Garcı́a-Martı́nez, León F.; Gaynor, Richard B.

doi:10.1093/emboj/16.6.1224

Cited by 133 publications

(126 citation statements)

References 75 publications

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“…Although these analyses hinted that Nullbasic might be successfully delivered to target cells by lentiviral vectors, overall transduction ability of the lentiviral particles conveying Nullbasic were markedly reduced compared with controls, an outcome that could be largely attributed to a defect in reverse transcription. However, Nullbasic did not affect infectivity of MLV-A virus-like particles, indicating that Nullbasic most likely targets the HIV-1 reverse transcription complex (RTC), cellular components important for HIV-1 reverse transcription, or may act as a trans-dominant negative inhibitor given evidence that Tat can support improved HIV-1 reverse transcription (Harrich et al, 1997). The precise mechanism by which Nullbasic inhibits reverse transcription remains to be determined.…”

Section: Discussionmentioning

confidence: 99%

A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4⁺T Cells

et al. 2013

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Here we show potent inhibition of HIV-1 replication in a human T cell line and primary human CD4+ cells by expressing a single antiviral protein. Nullbasic is a mutant form of the HIV-1 Tat protein that was previously shown to strongly inhibit HIV-1 replication in nonhematopoietic cell lines by targeting three steps of HIV-1 replication: reverse transcription, transport of viral mRNA, and trans-activation of HIV-1 gene expression. Here we investigated gene delivery of Nullbasic, using lentiviral and retroviral vectors. Although Nullbasic could be delivered by lentiviral vectors to target cells, transduction efficiencies were sharply reduced primarily because of negative effects on reverse transcription mediated by Nullbasic. However, Nullbasic did not inhibit transduction of HEK293T cells by a murine leukemia virus (MLV)-based retroviral vector. Therefore, MLV-based virus-like particles were used to transduce and express Nullbasic-EGFP or EGFP in Jurkat cells, a human leukemia T cell line, and Nullbasic-ZsGreen1 or ZsGreen1 in primary human CD4 + cells. HIV-1 replication kinetics were similar in parental Jurkat and Jurkat-EGFP cells, but were strongly attenuated in Jurkat-Nullbasic-EGFP cells. Similarly, virus replication in primary CD4+ cells expressing a Nullbasic-ZsGreen1 fusion protein was inhibited by approximately 8-to 10-fold. These experiments demonstrate the potential of Nullbasic, which has unique inhibitory activity, as an antiviral agent against HIV-1 infection.

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Section: Discussionmentioning

confidence: 99%

A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4⁺T Cells

et al. 2013

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“…The secondary structure of TAR consists of two helical stem regions separated by three unpaired bases that form an internal bulge, and the terminal stem is capped by a 6-nt apical loop. Upon Tat binding to TAR, viral mRNA production is increased several hundredfold through a resulting increase in the elongation capacity of RNA polymerase (Harrich et al 1996(Harrich et al , 1997. Binding of Tat to TAR is mediated by a single arginine residue located in the basic portion of the protein (Calnan et al 1991a,b).…”

Section: Introductionmentioning

confidence: 99%

Ligand-induced changes in 2-aminopurine fluorescence as a probe for small molecule binding to HIV-1 TAR RNA

Bradrick¹,

Marino²

2004

RNA

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“…Tat is a multifunctional protein, absolutely required for virus replication and AIDS progression. Besides its primary function as the viral transcription factor, Tat has been proposed to be required for efficient reverse transcription (1). Tat is secreted from infected cells (2,3), whereupon it binds to neighboring cells through electrostatic interactions, chemokine receptors (4), or cell surface integrins (5).…”

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confidence: 99%

Tat Acetyl-acceptor Lysines Are Important for Human Immunodeficiency Virus Type-1 Replication

Brès

Kiernan

Emiliani

et al. 2002

Journal of Biological Chemistry

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The human immunodeficiency virus type-1 trans-activator Tat is a transcription factor that activates the HIV-1 promoter through binding to the trans-activationresponsive region (TAR) localized at the 5-end of all viral transcripts. We and others have recently shown that Tat is directly acetylated at lysine 28, within the activation domain, and lysine 50, in the TAR RNA binding domain, by Tat-associated histone acetyltransferases p300, p300/CBP-associating factor, and hGCN5. Here, we show that mutation of acetyl-acceptor lysines to arginine or glutamine affects virus replication. Interestingly, mutation of lysine 28 and lysine 50 differentially affected Tat trans-activation of integrated versus nonintegrated long terminal repeat. Our results highlight the importance of lysine 28 and lysine 50 of Tat in virus replication and Tat-mediated trans-activation.

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Tat is required for efficient HIV-1 reverse transcription

Cited by 133 publications

References 75 publications

A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4⁺T Cells

A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4⁺T Cells

Ligand-induced changes in 2-aminopurine fluorescence as a probe for small molecule binding to HIV-1 TAR RNA

Tat Acetyl-acceptor Lysines Are Important for Human Immunodeficiency Virus Type-1 Replication

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Tat is required for efficient HIV-1 reverse transcription

Cited by 133 publications

References 75 publications

A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4+T Cells

A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4+T Cells

Ligand-induced changes in 2-aminopurine fluorescence as a probe for small molecule binding to HIV-1 TAR RNA

Tat Acetyl-acceptor Lysines Are Important for Human Immunodeficiency Virus Type-1 Replication

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A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4⁺T Cells

A Mutant Tat Protein Provides Strong Protection from HIV-1 Infection in Human CD4⁺T Cells