Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments

It is well documented that influenza A viruses selectively package 8 distinct viral ribonucleoprotein complexes (vRNPs) into each virion; however, the role of host factors in genome assembly is not completely understood. To evaluate the significance of cellular factors in genome assembly, we generat...

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Autores principales: Han, Julianna, Ganti, Ketaki, Sali, Veeresh Kumar, Twigg, Carly, Zhang, Yifeng, Manivasagam, Senthamizharasi, Liang, Chieh-Yu, Vogel, Olivia A., Huang, Iris, Emmanuel, Shanan N., Plung, Jesse, Radoshevich, Lillianna, Perez, Jasmine T., Lowen, Anice C., Manicassamy, Balaji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8136845/
https://www.ncbi.nlm.nih.gov/pubmed/33970958
http://dx.doi.org/10.1371/journal.ppat.1009517
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author Han, Julianna
Ganti, Ketaki
Sali, Veeresh Kumar
Twigg, Carly
Zhang, Yifeng
Manivasagam, Senthamizharasi
Liang, Chieh-Yu
Vogel, Olivia A.
Huang, Iris
Emmanuel, Shanan N.
Plung, Jesse
Radoshevich, Lillianna
Perez, Jasmine T.
Lowen, Anice C.
Manicassamy, Balaji
author_facet Han, Julianna
Ganti, Ketaki
Sali, Veeresh Kumar
Twigg, Carly
Zhang, Yifeng
Manivasagam, Senthamizharasi
Liang, Chieh-Yu
Vogel, Olivia A.
Huang, Iris
Emmanuel, Shanan N.
Plung, Jesse
Radoshevich, Lillianna
Perez, Jasmine T.
Lowen, Anice C.
Manicassamy, Balaji
author_sort Han, Julianna
collection PubMed
description It is well documented that influenza A viruses selectively package 8 distinct viral ribonucleoprotein complexes (vRNPs) into each virion; however, the role of host factors in genome assembly is not completely understood. To evaluate the significance of cellular factors in genome assembly, we generated a reporter virus carrying a tetracysteine tag in the NP gene (NP-Tc virus) and assessed the dynamics of vRNP localization with cellular components by fluorescence microscopy. At early time points, vRNP complexes were preferentially exported to the MTOC; subsequently, vRNPs associated on vesicles positive for cellular factor Rab11a and formed distinct vRNP bundles that trafficked to the plasma membrane on microtubule networks. In Rab11a deficient cells, however, vRNP bundles were smaller in the cytoplasm with less co-localization between different vRNP segments. Furthermore, Rab11a deficiency increased the production of non-infectious particles with higher RNA copy number to PFU ratios, indicative of defects in specific genome assembly. These results indicate that Rab11a+ vesicles serve as hubs for the congregation of vRNP complexes and enable specific genome assembly through vRNP:vRNP interactions, revealing the importance of Rab11a as a critical host factor for influenza A virus genome assembly.
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spelling pubmed-81368452021-06-02 Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments Han, Julianna Ganti, Ketaki Sali, Veeresh Kumar Twigg, Carly Zhang, Yifeng Manivasagam, Senthamizharasi Liang, Chieh-Yu Vogel, Olivia A. Huang, Iris Emmanuel, Shanan N. Plung, Jesse Radoshevich, Lillianna Perez, Jasmine T. Lowen, Anice C. Manicassamy, Balaji PLoS Pathog Research Article It is well documented that influenza A viruses selectively package 8 distinct viral ribonucleoprotein complexes (vRNPs) into each virion; however, the role of host factors in genome assembly is not completely understood. To evaluate the significance of cellular factors in genome assembly, we generated a reporter virus carrying a tetracysteine tag in the NP gene (NP-Tc virus) and assessed the dynamics of vRNP localization with cellular components by fluorescence microscopy. At early time points, vRNP complexes were preferentially exported to the MTOC; subsequently, vRNPs associated on vesicles positive for cellular factor Rab11a and formed distinct vRNP bundles that trafficked to the plasma membrane on microtubule networks. In Rab11a deficient cells, however, vRNP bundles were smaller in the cytoplasm with less co-localization between different vRNP segments. Furthermore, Rab11a deficiency increased the production of non-infectious particles with higher RNA copy number to PFU ratios, indicative of defects in specific genome assembly. These results indicate that Rab11a+ vesicles serve as hubs for the congregation of vRNP complexes and enable specific genome assembly through vRNP:vRNP interactions, revealing the importance of Rab11a as a critical host factor for influenza A virus genome assembly. Public Library of Science 2021-05-10 /pmc/articles/PMC8136845/ /pubmed/33970958 http://dx.doi.org/10.1371/journal.ppat.1009517 Text en © 2021 Han et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Han, Julianna
Ganti, Ketaki
Sali, Veeresh Kumar
Twigg, Carly
Zhang, Yifeng
Manivasagam, Senthamizharasi
Liang, Chieh-Yu
Vogel, Olivia A.
Huang, Iris
Emmanuel, Shanan N.
Plung, Jesse
Radoshevich, Lillianna
Perez, Jasmine T.
Lowen, Anice C.
Manicassamy, Balaji
Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments
title Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments
title_full Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments
title_fullStr Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments
title_full_unstemmed Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments
title_short Host factor Rab11a is critical for efficient assembly of influenza A virus genomic segments
title_sort host factor rab11a is critical for efficient assembly of influenza a virus genomic segments
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8136845/
https://www.ncbi.nlm.nih.gov/pubmed/33970958
http://dx.doi.org/10.1371/journal.ppat.1009517
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