Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target

Reverse transcription is the central defining feature of HIV-1 replication. We previously reported that the cellular eukaryotic elongation factor 1 (eEF1) complex associates with the HIV-1 reverse transcription complex (RTC) and the association is important for late steps of reverse transcription. H...

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Autores principales: Li, Dongsheng, Wei, Ting, Rawle, Daniel J., Qin, Fangyun, Wang, Rui, Soares, Dinesh C., Jin, Hongping, Sivakumaran, Haran, Lin, Min-Hsuan, Spann, Kirsten, Abbott, Catherine M., Harrich, David
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4666417/
https://www.ncbi.nlm.nih.gov/pubmed/26624286
http://dx.doi.org/10.1371/journal.ppat.1005289
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author Li, Dongsheng
Wei, Ting
Rawle, Daniel J.
Qin, Fangyun
Wang, Rui
Soares, Dinesh C.
Jin, Hongping
Sivakumaran, Haran
Lin, Min-Hsuan
Spann, Kirsten
Abbott, Catherine M.
Harrich, David
author_facet Li, Dongsheng
Wei, Ting
Rawle, Daniel J.
Qin, Fangyun
Wang, Rui
Soares, Dinesh C.
Jin, Hongping
Sivakumaran, Haran
Lin, Min-Hsuan
Spann, Kirsten
Abbott, Catherine M.
Harrich, David
author_sort Li, Dongsheng
collection PubMed
description Reverse transcription is the central defining feature of HIV-1 replication. We previously reported that the cellular eukaryotic elongation factor 1 (eEF1) complex associates with the HIV-1 reverse transcription complex (RTC) and the association is important for late steps of reverse transcription. Here we show that association between the eEF1 and RTC complexes occurs by a strong and direct interaction between the subunit eEF1A and reverse transcriptase (RT). Using biolayer interferometry and co-immunoprecipitation (co-IP) assays, we show that association between the eEF1 and RTC complexes occurs by a strong (K(D) ~3–4 nM) and direct interaction between eEF1A and reverse transcriptase (RT). Biolayer interferometry analysis of cell lysates with titrated levels of eEF1A indicates it is a predominant cellular RT binding protein. Both the RT thumb and connection domains are required for interaction with eEF1A. A single amino acid mutation, W252A, within the thumb domain impaired co-IP between eEF1A and RT, and also significantly reduced the efficiency of late reverse transcription and virus replication when incorporated into infectious HIV-1. Molecular modeling analysis indicated that interaction between W252 and L303 are important for RT structure, and their mutation to alanine did not impair heterodimerisation, but negatively impacted interaction with eEF1A. Didemnin B, which specifically binds eEF1A, potently inhibited HIV-1 reverse transcription by greater than 2 logs at subnanomolar concentrations, especially affecting reverse transcription late DNA synthesis. Analysis showed reduced levels of RTCs from HIV-1-infected HEK293T treated with didemnin B compared to untreated cells. Interestingly, HIV-1 with a W252A RT mutation was resistant to didemnin B negative effects showing that didemnin B affects HIV-1 by targeting the RT-eEF1A interaction. The combined evidence indicates a direct interaction between eEF1A and RT is crucial for HIV reverse transcription and replication, and the RT-eEF1A interaction is a potential drug target.
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spelling pubmed-46664172015-12-10 Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target Li, Dongsheng Wei, Ting Rawle, Daniel J. Qin, Fangyun Wang, Rui Soares, Dinesh C. Jin, Hongping Sivakumaran, Haran Lin, Min-Hsuan Spann, Kirsten Abbott, Catherine M. Harrich, David PLoS Pathog Research Article Reverse transcription is the central defining feature of HIV-1 replication. We previously reported that the cellular eukaryotic elongation factor 1 (eEF1) complex associates with the HIV-1 reverse transcription complex (RTC) and the association is important for late steps of reverse transcription. Here we show that association between the eEF1 and RTC complexes occurs by a strong and direct interaction between the subunit eEF1A and reverse transcriptase (RT). Using biolayer interferometry and co-immunoprecipitation (co-IP) assays, we show that association between the eEF1 and RTC complexes occurs by a strong (K(D) ~3–4 nM) and direct interaction between eEF1A and reverse transcriptase (RT). Biolayer interferometry analysis of cell lysates with titrated levels of eEF1A indicates it is a predominant cellular RT binding protein. Both the RT thumb and connection domains are required for interaction with eEF1A. A single amino acid mutation, W252A, within the thumb domain impaired co-IP between eEF1A and RT, and also significantly reduced the efficiency of late reverse transcription and virus replication when incorporated into infectious HIV-1. Molecular modeling analysis indicated that interaction between W252 and L303 are important for RT structure, and their mutation to alanine did not impair heterodimerisation, but negatively impacted interaction with eEF1A. Didemnin B, which specifically binds eEF1A, potently inhibited HIV-1 reverse transcription by greater than 2 logs at subnanomolar concentrations, especially affecting reverse transcription late DNA synthesis. Analysis showed reduced levels of RTCs from HIV-1-infected HEK293T treated with didemnin B compared to untreated cells. Interestingly, HIV-1 with a W252A RT mutation was resistant to didemnin B negative effects showing that didemnin B affects HIV-1 by targeting the RT-eEF1A interaction. The combined evidence indicates a direct interaction between eEF1A and RT is crucial for HIV reverse transcription and replication, and the RT-eEF1A interaction is a potential drug target. Public Library of Science 2015-12-01 /pmc/articles/PMC4666417/ /pubmed/26624286 http://dx.doi.org/10.1371/journal.ppat.1005289 Text en © 2015 Li et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Li, Dongsheng
Wei, Ting
Rawle, Daniel J.
Qin, Fangyun
Wang, Rui
Soares, Dinesh C.
Jin, Hongping
Sivakumaran, Haran
Lin, Min-Hsuan
Spann, Kirsten
Abbott, Catherine M.
Harrich, David
Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target
title Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target
title_full Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target
title_fullStr Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target
title_full_unstemmed Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target
title_short Specific Interaction between eEF1A and HIV RT Is Critical for HIV-1 Reverse Transcription and a Potential Anti-HIV Target
title_sort specific interaction between eef1a and hiv rt is critical for hiv-1 reverse transcription and a potential anti-hiv target
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4666417/
https://www.ncbi.nlm.nih.gov/pubmed/26624286
http://dx.doi.org/10.1371/journal.ppat.1005289
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