H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1

Virus–host interactions play vital roles in viral replication and virus-induced pathogenesis. Viruses rely entirely upon host cells to reproduce progeny viruses; however, host factors positively or negatively regulate virus replication by interacting with viral proteins. The elucidation of virus–hos...

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Autores principales: Kudoh, Ayumi, Miyakawa, Kei, Matsunaga, Satoko, Matsushima, Yuki, Kosugi, Isao, Kimura, Hirokazu, Hayakawa, Satoshi, Sawasaki, Tatsuya, Ryo, Akihide
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2016
Materias:
Microbiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4904303/
https://www.ncbi.nlm.nih.gov/pubmed/27379031
http://dx.doi.org/10.3389/fmicb.2016.00883
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author Kudoh, Ayumi
Miyakawa, Kei
Matsunaga, Satoko
Matsushima, Yuki
Kosugi, Isao
Kimura, Hirokazu
Hayakawa, Satoshi
Sawasaki, Tatsuya
Ryo, Akihide
author_facet Kudoh, Ayumi
Miyakawa, Kei
Matsunaga, Satoko
Matsushima, Yuki
Kosugi, Isao
Kimura, Hirokazu
Hayakawa, Satoshi
Sawasaki, Tatsuya
Ryo, Akihide
author_sort Kudoh, Ayumi
collection PubMed
description Virus–host interactions play vital roles in viral replication and virus-induced pathogenesis. Viruses rely entirely upon host cells to reproduce progeny viruses; however, host factors positively or negatively regulate virus replication by interacting with viral proteins. The elucidation of virus–host protein interaction not only provides a better understanding of the molecular mechanisms by which host cells combat viral infections, but also facilitates the development of new anti-viral therapeutics. Identification of relevant host factors requires techniques that enable comprehensive characterization of virus–host protein interactions. In this study, we developed a proteomic approach to systematically identify human protein kinases that interact potently with viral proteins. For this purpose, we synthesized 412 full-length human protein kinases using the wheat germ cell-free protein synthesis system, and screened them for their association with a virus protein using the amplified luminescent proximity homogenous assay (AlphaScreen). Using this system, we attempted to discover a robust anti-viral host restriction mechanism targeting virus protein X (Vpx) of HIV-2. The screen identified H11/HSPB8 as a Vpx-binding protein that negatively regulates the stability and function of Vpx. Indeed, overexpression of H11/HSPB8 promoted the degradation of Vpx via the ubiquitin–proteasome pathway and inhibited its interaction with SAMHD1, a host restriction factor responsible for blocking replication of HIV. Conversely, targeted knockdown of H11/HSPB8 in human trophoblast cells, which ordinarily express high levels of this protein, restored the expression and function of Vpx, making the cells highly susceptible to viral replication. These results demonstrate that our proteomic approach represents a powerful tool for revealing virus–host interaction not yet identified by conventional methods. Furthermore, we showed that H11/HSPB8 could be a potential host regulatory factor that may prevent placental infection of HIV-2 during pregnancy.
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spelling pubmed-49043032016-07-04 H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1 Kudoh, Ayumi Miyakawa, Kei Matsunaga, Satoko Matsushima, Yuki Kosugi, Isao Kimura, Hirokazu Hayakawa, Satoshi Sawasaki, Tatsuya Ryo, Akihide Front Microbiol Microbiology Virus–host interactions play vital roles in viral replication and virus-induced pathogenesis. Viruses rely entirely upon host cells to reproduce progeny viruses; however, host factors positively or negatively regulate virus replication by interacting with viral proteins. The elucidation of virus–host protein interaction not only provides a better understanding of the molecular mechanisms by which host cells combat viral infections, but also facilitates the development of new anti-viral therapeutics. Identification of relevant host factors requires techniques that enable comprehensive characterization of virus–host protein interactions. In this study, we developed a proteomic approach to systematically identify human protein kinases that interact potently with viral proteins. For this purpose, we synthesized 412 full-length human protein kinases using the wheat germ cell-free protein synthesis system, and screened them for their association with a virus protein using the amplified luminescent proximity homogenous assay (AlphaScreen). Using this system, we attempted to discover a robust anti-viral host restriction mechanism targeting virus protein X (Vpx) of HIV-2. The screen identified H11/HSPB8 as a Vpx-binding protein that negatively regulates the stability and function of Vpx. Indeed, overexpression of H11/HSPB8 promoted the degradation of Vpx via the ubiquitin–proteasome pathway and inhibited its interaction with SAMHD1, a host restriction factor responsible for blocking replication of HIV. Conversely, targeted knockdown of H11/HSPB8 in human trophoblast cells, which ordinarily express high levels of this protein, restored the expression and function of Vpx, making the cells highly susceptible to viral replication. These results demonstrate that our proteomic approach represents a powerful tool for revealing virus–host interaction not yet identified by conventional methods. Furthermore, we showed that H11/HSPB8 could be a potential host regulatory factor that may prevent placental infection of HIV-2 during pregnancy. Frontiers Media S.A. 2016-06-13 /pmc/articles/PMC4904303/ /pubmed/27379031 http://dx.doi.org/10.3389/fmicb.2016.00883 Text en Copyright © 2016 Kudoh, Miyakawa, Matsunaga, Matsushima, Kosugi, Kimura, Hayakawa, Sawasaki and Ryo. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Microbiology
Kudoh, Ayumi
Miyakawa, Kei
Matsunaga, Satoko
Matsushima, Yuki
Kosugi, Isao
Kimura, Hirokazu
Hayakawa, Satoshi
Sawasaki, Tatsuya
Ryo, Akihide
H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1
title H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1
title_full H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1
title_fullStr H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1
title_full_unstemmed H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1
title_short H11/HSPB8 Restricts HIV-2 Vpx to Restore the Anti-Viral Activity of SAMHD1
title_sort h11/hspb8 restricts hiv-2 vpx to restore the anti-viral activity of samhd1
topic Microbiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4904303/
https://www.ncbi.nlm.nih.gov/pubmed/27379031
http://dx.doi.org/10.3389/fmicb.2016.00883
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