A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection

The large nucleoporin Nup358/RanBP2 forms eight filaments that project from the nuclear pore into the cytoplasm where they function as docking platforms for nucleocytoplasmic transport receptors. RNAi screens have implicated Nup358 in the HIV-1 life cycle. The 164 C-terminal amino acids of this 3,22...

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Autores principales: Meehan, Anne M., Saenz, Dyana T., Guevera, Rebekah, Morrison, James H., Peretz, Mary, Fadel, Hind J., Hamada, Masakazu, van Deursen, Jan, Poeschla, Eric M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3930637/
https://www.ncbi.nlm.nih.gov/pubmed/24586169
http://dx.doi.org/10.1371/journal.ppat.1003969
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author Meehan, Anne M.
Saenz, Dyana T.
Guevera, Rebekah
Morrison, James H.
Peretz, Mary
Fadel, Hind J.
Hamada, Masakazu
van Deursen, Jan
Poeschla, Eric M.
author_facet Meehan, Anne M.
Saenz, Dyana T.
Guevera, Rebekah
Morrison, James H.
Peretz, Mary
Fadel, Hind J.
Hamada, Masakazu
van Deursen, Jan
Poeschla, Eric M.
author_sort Meehan, Anne M.
collection PubMed
description The large nucleoporin Nup358/RanBP2 forms eight filaments that project from the nuclear pore into the cytoplasm where they function as docking platforms for nucleocytoplasmic transport receptors. RNAi screens have implicated Nup358 in the HIV-1 life cycle. The 164 C-terminal amino acids of this 3,224 amino acid protein are a cyclophilin homology domain (Nup358Cyp), which has potential to bind the HIV-1 capsid and regulate viral progress to integration. Here we examined the virological role of Nup358 in conditional knockout mouse cells and in RNAi-depleted human CD4+ T cells. Cre-mediated gene knockout was toxic and diminished HIV-1 infectivity. However, cellular health and HIV-1 susceptibility were coordinately preserved if, prior to gene inactivation, a transposon was used to express all of Nup358 or only the N-terminal 1340 amino acids that contain three FG repeats and a Ran-binding domain. HIV-1, but not N74D capsid-mutant HIV-1, was markedly sensitive to TNPO3 depletion, but they infected 1–1340 segment-complemented Nup358 knockout cells equivalently. Human and mouse CypA both rescued HIV-1 in CypA gene −/− Jurkat cells and TRIM-Nup358Cyp fusions derived from each species were equally antiviral; each also inhibited both WT and N74D virus. In the human CD4+ T cell line SupT1, abrupt Nup358 depletion reduced viral replication but stable Nup358-depleted cells replicated HIV-1 normally. Thus, human CD4+ T cells can accommodate to loss of Nup358 and preserve HIV-1 susceptibility. Experiments with cylosporine, viruses with capsids that do not bind cyclophilins, and growth arrest did not uncover viral dependency on the C-terminal domains of Nup358. Our data reinforce the virological importance of TNPO3 and show that Nup358 supports nuclear transport functions important for cellular homeostasis and for HIV-1 nuclear import. However, the results do not suggest direct roles for the Nup358 cyclophilin or SUMO E3 ligase domains in engaging the HIV-1 capsid prior to nuclear translocation.
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spelling pubmed-39306372014-02-25 A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection Meehan, Anne M. Saenz, Dyana T. Guevera, Rebekah Morrison, James H. Peretz, Mary Fadel, Hind J. Hamada, Masakazu van Deursen, Jan Poeschla, Eric M. PLoS Pathog Research Article The large nucleoporin Nup358/RanBP2 forms eight filaments that project from the nuclear pore into the cytoplasm where they function as docking platforms for nucleocytoplasmic transport receptors. RNAi screens have implicated Nup358 in the HIV-1 life cycle. The 164 C-terminal amino acids of this 3,224 amino acid protein are a cyclophilin homology domain (Nup358Cyp), which has potential to bind the HIV-1 capsid and regulate viral progress to integration. Here we examined the virological role of Nup358 in conditional knockout mouse cells and in RNAi-depleted human CD4+ T cells. Cre-mediated gene knockout was toxic and diminished HIV-1 infectivity. However, cellular health and HIV-1 susceptibility were coordinately preserved if, prior to gene inactivation, a transposon was used to express all of Nup358 or only the N-terminal 1340 amino acids that contain three FG repeats and a Ran-binding domain. HIV-1, but not N74D capsid-mutant HIV-1, was markedly sensitive to TNPO3 depletion, but they infected 1–1340 segment-complemented Nup358 knockout cells equivalently. Human and mouse CypA both rescued HIV-1 in CypA gene −/− Jurkat cells and TRIM-Nup358Cyp fusions derived from each species were equally antiviral; each also inhibited both WT and N74D virus. In the human CD4+ T cell line SupT1, abrupt Nup358 depletion reduced viral replication but stable Nup358-depleted cells replicated HIV-1 normally. Thus, human CD4+ T cells can accommodate to loss of Nup358 and preserve HIV-1 susceptibility. Experiments with cylosporine, viruses with capsids that do not bind cyclophilins, and growth arrest did not uncover viral dependency on the C-terminal domains of Nup358. Our data reinforce the virological importance of TNPO3 and show that Nup358 supports nuclear transport functions important for cellular homeostasis and for HIV-1 nuclear import. However, the results do not suggest direct roles for the Nup358 cyclophilin or SUMO E3 ligase domains in engaging the HIV-1 capsid prior to nuclear translocation. Public Library of Science 2014-02-20 /pmc/articles/PMC3930637/ /pubmed/24586169 http://dx.doi.org/10.1371/journal.ppat.1003969 Text en © 2014 Meehan 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
Meehan, Anne M.
Saenz, Dyana T.
Guevera, Rebekah
Morrison, James H.
Peretz, Mary
Fadel, Hind J.
Hamada, Masakazu
van Deursen, Jan
Poeschla, Eric M.
A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection
title A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection
title_full A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection
title_fullStr A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection
title_full_unstemmed A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection
title_short A Cyclophilin Homology Domain-Independent Role for Nup358 in HIV-1 Infection
title_sort cyclophilin homology domain-independent role for nup358 in hiv-1 infection
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3930637/
https://www.ncbi.nlm.nih.gov/pubmed/24586169
http://dx.doi.org/10.1371/journal.ppat.1003969
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