The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase

Previously, we reported that an HIV-1 variant containing Met-to-Ile change at codon 50 and Val-to-Ile mutation at codon 151 of integrase (IN), HIV(IN:M50I/V151I), was an impaired virus. Despite the mutations being in IN, the virus release was significantly suppressed (p < 0.0001) and the initiati...

Descripción completa

Detalles Bibliográficos
Autores principales: Imamichi, Tomozumi, Chen, Qian, Hao, Ming, Chang, Weizhong, Yang, Jun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9788298/
https://www.ncbi.nlm.nih.gov/pubmed/36560691
http://dx.doi.org/10.3390/v14122687
_version_ 1784858720398737408
author Imamichi, Tomozumi
Chen, Qian
Hao, Ming
Chang, Weizhong
Yang, Jun
author_facet Imamichi, Tomozumi
Chen, Qian
Hao, Ming
Chang, Weizhong
Yang, Jun
author_sort Imamichi, Tomozumi
collection PubMed
description Previously, we reported that an HIV-1 variant containing Met-to-Ile change at codon 50 and Val-to-Ile mutation at codon 151 of integrase (IN), HIV(IN:M50I/V151I), was an impaired virus. Despite the mutations being in IN, the virus release was significantly suppressed (p < 0.0001) and the initiation of autoprocessing was inhibited; the mechanism of the defect remains unknown. In the current study, we attempted to identify the critical domains or amino acid (aa) residue(s) that promote defects in HIV(IN:M50I/V151I), using a series of variants, including truncated or aa-substituted RNase H (RH) or IN. The results demonstrated that virus release and the initiation of autoprocessing were regulated by the C-terminal domains (CTDs) of RH and IN. Further studies illustrated that Asp at codon 109 of RH CTD and Asp at the C terminus of IN induces the defect. This result indicated that the CTDs of RH and IN in GagPol and particular aa positions in RH and IN regulated the virus release and the initiation of autoprocessing, and these sites could be potential targets for the development of new therapies.
format Online
Article
Text
id pubmed-9788298
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-97882982022-12-24 The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase Imamichi, Tomozumi Chen, Qian Hao, Ming Chang, Weizhong Yang, Jun Viruses Article Previously, we reported that an HIV-1 variant containing Met-to-Ile change at codon 50 and Val-to-Ile mutation at codon 151 of integrase (IN), HIV(IN:M50I/V151I), was an impaired virus. Despite the mutations being in IN, the virus release was significantly suppressed (p < 0.0001) and the initiation of autoprocessing was inhibited; the mechanism of the defect remains unknown. In the current study, we attempted to identify the critical domains or amino acid (aa) residue(s) that promote defects in HIV(IN:M50I/V151I), using a series of variants, including truncated or aa-substituted RNase H (RH) or IN. The results demonstrated that virus release and the initiation of autoprocessing were regulated by the C-terminal domains (CTDs) of RH and IN. Further studies illustrated that Asp at codon 109 of RH CTD and Asp at the C terminus of IN induces the defect. This result indicated that the CTDs of RH and IN in GagPol and particular aa positions in RH and IN regulated the virus release and the initiation of autoprocessing, and these sites could be potential targets for the development of new therapies. MDPI 2022-11-30 /pmc/articles/PMC9788298/ /pubmed/36560691 http://dx.doi.org/10.3390/v14122687 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Imamichi, Tomozumi
Chen, Qian
Hao, Ming
Chang, Weizhong
Yang, Jun
The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase
title The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase
title_full The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase
title_fullStr The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase
title_full_unstemmed The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase
title_short The C-Terminal Domain of RNase H and the C-Terminus Amino Acid Residue Regulate Virus Release and Autoprocessing of a Defective HIV-1 Possessing M50I and V151I Changes in Integrase
title_sort c-terminal domain of rnase h and the c-terminus amino acid residue regulate virus release and autoprocessing of a defective hiv-1 possessing m50i and v151i changes in integrase
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9788298/
https://www.ncbi.nlm.nih.gov/pubmed/36560691
http://dx.doi.org/10.3390/v14122687
work_keys_str_mv AT imamichitomozumi thecterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT chenqian thecterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT haoming thecterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT changweizhong thecterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT yangjun thecterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT imamichitomozumi cterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT chenqian cterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT haoming cterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT changweizhong cterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase
AT yangjun cterminaldomainofrnasehandthecterminusaminoacidresidueregulatevirusreleaseandautoprocessingofadefectivehiv1possessingm50iandv151ichangesinintegrase

Ejemplares similares