Defining the HIV Capsid Binding Site of Nucleoporin 153

The interaction between the HIV-1 capsid and human nucleoporin 153 (NUP153) is vital for delivering the HIV-1 preintegration complex into the nucleus via the nuclear pore complex. The interaction with the capsid requires a phenylalanine/glycine-containing motif in the C-terminus of NUP153 (NUP153C)....

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Autores principales: Li, Shunji, Patel, Jagdish Suresh, Yang, Jordan, Crabtree, Angela Marie, Rubenstein, Brenda Marilyn, Lund-Andersen, Peik Karl, Ytreberg, Frederick Marty, Rowley, Paul Andrew
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9599535/
https://www.ncbi.nlm.nih.gov/pubmed/36040047
http://dx.doi.org/10.1128/msphere.00310-22
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author Li, Shunji
Patel, Jagdish Suresh
Yang, Jordan
Crabtree, Angela Marie
Rubenstein, Brenda Marilyn
Lund-Andersen, Peik Karl
Ytreberg, Frederick Marty
Rowley, Paul Andrew
author_facet Li, Shunji
Patel, Jagdish Suresh
Yang, Jordan
Crabtree, Angela Marie
Rubenstein, Brenda Marilyn
Lund-Andersen, Peik Karl
Ytreberg, Frederick Marty
Rowley, Paul Andrew
author_sort Li, Shunji
collection PubMed
description The interaction between the HIV-1 capsid and human nucleoporin 153 (NUP153) is vital for delivering the HIV-1 preintegration complex into the nucleus via the nuclear pore complex. The interaction with the capsid requires a phenylalanine/glycine-containing motif in the C-terminus of NUP153 (NUP153C). This study used molecular modeling and biochemical assays to comprehensively determine the amino acids in NUP153 that are important for capsid interaction. Molecular dynamics, FoldX, and PyRosetta simulations delineated the minimal capsid binding motif of NUP153 based on the known structure of NUP153 bound to the HIV-1 capsid hexamer. Computational predictions were experimentally validated by testing the interaction of NUP153 with capsid using an in vitro binding assay and a cell-based TRIM-NUP153C restriction assay. This work identified eight amino acids from P1411 to G1418 that stably engage with capsid, with significant correlations between the interactions predicted by molecular models and empirical experiments. This validated the usefulness of this multidisciplinary approach to rapidly characterize the interaction between human proteins and the HIV-1 capsid. IMPORTANCE The human immunodeficiency virus (HIV) can infect nondividing cells by interacting with the host nuclear pore complex. The host nuclear pore protein NUP153 directly interacts with the HIV capsid to promote viral nuclear entry. This study used a multidisciplinary approach combining computational and experimental techniques to comprehensively map the effect of mutating the amino acids of NUP153 on HIV capsid interaction. This work showed a significant correlation between computational and empirical data sets, revealing that the HIV capsid interacted specifically with only six amino acids of NUP153. The simplicity of the interaction motif suggested other FG-containing motifs could also interact with the HIV-1 capsid. Furthermore, it was predicted that naturally occurring polymorphisms in human and nonhuman primates would disrupt NUP153 interaction with capsid, potentially protecting certain populations from HIV-1 infection.
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spelling pubmed-95995352022-10-27 Defining the HIV Capsid Binding Site of Nucleoporin 153 Li, Shunji Patel, Jagdish Suresh Yang, Jordan Crabtree, Angela Marie Rubenstein, Brenda Marilyn Lund-Andersen, Peik Karl Ytreberg, Frederick Marty Rowley, Paul Andrew mSphere Research Article The interaction between the HIV-1 capsid and human nucleoporin 153 (NUP153) is vital for delivering the HIV-1 preintegration complex into the nucleus via the nuclear pore complex. The interaction with the capsid requires a phenylalanine/glycine-containing motif in the C-terminus of NUP153 (NUP153C). This study used molecular modeling and biochemical assays to comprehensively determine the amino acids in NUP153 that are important for capsid interaction. Molecular dynamics, FoldX, and PyRosetta simulations delineated the minimal capsid binding motif of NUP153 based on the known structure of NUP153 bound to the HIV-1 capsid hexamer. Computational predictions were experimentally validated by testing the interaction of NUP153 with capsid using an in vitro binding assay and a cell-based TRIM-NUP153C restriction assay. This work identified eight amino acids from P1411 to G1418 that stably engage with capsid, with significant correlations between the interactions predicted by molecular models and empirical experiments. This validated the usefulness of this multidisciplinary approach to rapidly characterize the interaction between human proteins and the HIV-1 capsid. IMPORTANCE The human immunodeficiency virus (HIV) can infect nondividing cells by interacting with the host nuclear pore complex. The host nuclear pore protein NUP153 directly interacts with the HIV capsid to promote viral nuclear entry. This study used a multidisciplinary approach combining computational and experimental techniques to comprehensively map the effect of mutating the amino acids of NUP153 on HIV capsid interaction. This work showed a significant correlation between computational and empirical data sets, revealing that the HIV capsid interacted specifically with only six amino acids of NUP153. The simplicity of the interaction motif suggested other FG-containing motifs could also interact with the HIV-1 capsid. Furthermore, it was predicted that naturally occurring polymorphisms in human and nonhuman primates would disrupt NUP153 interaction with capsid, potentially protecting certain populations from HIV-1 infection. American Society for Microbiology 2022-08-30 /pmc/articles/PMC9599535/ /pubmed/36040047 http://dx.doi.org/10.1128/msphere.00310-22 Text en Copyright © 2022 Li et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Li, Shunji
Patel, Jagdish Suresh
Yang, Jordan
Crabtree, Angela Marie
Rubenstein, Brenda Marilyn
Lund-Andersen, Peik Karl
Ytreberg, Frederick Marty
Rowley, Paul Andrew
Defining the HIV Capsid Binding Site of Nucleoporin 153
title Defining the HIV Capsid Binding Site of Nucleoporin 153
title_full Defining the HIV Capsid Binding Site of Nucleoporin 153
title_fullStr Defining the HIV Capsid Binding Site of Nucleoporin 153
title_full_unstemmed Defining the HIV Capsid Binding Site of Nucleoporin 153
title_short Defining the HIV Capsid Binding Site of Nucleoporin 153
title_sort defining the hiv capsid binding site of nucleoporin 153
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9599535/
https://www.ncbi.nlm.nih.gov/pubmed/36040047
http://dx.doi.org/10.1128/msphere.00310-22
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