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The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection

The signaling pathways and cellular functions regulated by the four Numb-associated kinases are largely unknown. We reported that AAK1 and GAK control intracellular trafficking of RNA viruses and revealed a requirement for BIKE in early and late stages of dengue virus (DENV) infection. However, the...

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Autores principales: Schor, Stanford, Pu, Szuyuan, Nicolaescu, Vlad, Azari, Siavash, Kõivomägi, Mardo, Karim, Marwah, Cassonnet, Patricia, Saul, Sirle, Neveu, Gregory, Yueh, Andrew, Demeret, Caroline, Skotheim, Jan M., Jacob, Yves, Randall, Glenn, Einav, Shirit
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9133654/
https://www.ncbi.nlm.nih.gov/pubmed/35452674
http://dx.doi.org/10.1016/j.jbc.2022.101956
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author Schor, Stanford
Pu, Szuyuan
Nicolaescu, Vlad
Azari, Siavash
Kõivomägi, Mardo
Karim, Marwah
Cassonnet, Patricia
Saul, Sirle
Neveu, Gregory
Yueh, Andrew
Demeret, Caroline
Skotheim, Jan M.
Jacob, Yves
Randall, Glenn
Einav, Shirit
author_facet Schor, Stanford
Pu, Szuyuan
Nicolaescu, Vlad
Azari, Siavash
Kõivomägi, Mardo
Karim, Marwah
Cassonnet, Patricia
Saul, Sirle
Neveu, Gregory
Yueh, Andrew
Demeret, Caroline
Skotheim, Jan M.
Jacob, Yves
Randall, Glenn
Einav, Shirit
author_sort Schor, Stanford
collection PubMed
description The signaling pathways and cellular functions regulated by the four Numb-associated kinases are largely unknown. We reported that AAK1 and GAK control intracellular trafficking of RNA viruses and revealed a requirement for BIKE in early and late stages of dengue virus (DENV) infection. However, the downstream targets phosphorylated by BIKE have not yet been identified. Here, to identify BIKE substrates, we conducted a barcode fusion genetics-yeast two-hybrid screen and retrieved publicly available data generated via affinity-purification mass spectrometry. We subsequently validated 19 of 47 putative BIKE interactors using mammalian cell–based protein–protein interaction assays. We found that CLINT1, a cargo-specific adapter implicated in bidirectional Golgi-to-endosome trafficking, emerged as a predominant hit in both screens. Our experiments indicated that BIKE catalyzes phosphorylation of a threonine 294 CLINT1 residue both in vitro and in cell culture. Our findings revealed that CLINT1 phosphorylation mediates its binding to the DENV nonstructural 3 protein and subsequently promotes DENV assembly and egress. Additionally, using live-cell imaging we revealed that CLINT1 cotraffics with DENV particles and is involved in mediating BIKE’s role in DENV infection. Finally, our data suggest that additional cellular BIKE interactors implicated in the host immune and stress responses and the ubiquitin proteasome system might also be candidate phosphorylation substrates of BIKE. In conclusion, these findings reveal cellular substrates and pathways regulated by the understudied Numb-associated kinase enzyme BIKE, a mechanism for CLINT1 regulation, and control of DENV infection via BIKE signaling, with potential implications for cell biology, virology, and host-targeted antiviral design.
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spelling pubmed-91336542022-06-04 The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection Schor, Stanford Pu, Szuyuan Nicolaescu, Vlad Azari, Siavash Kõivomägi, Mardo Karim, Marwah Cassonnet, Patricia Saul, Sirle Neveu, Gregory Yueh, Andrew Demeret, Caroline Skotheim, Jan M. Jacob, Yves Randall, Glenn Einav, Shirit J Biol Chem Research Article The signaling pathways and cellular functions regulated by the four Numb-associated kinases are largely unknown. We reported that AAK1 and GAK control intracellular trafficking of RNA viruses and revealed a requirement for BIKE in early and late stages of dengue virus (DENV) infection. However, the downstream targets phosphorylated by BIKE have not yet been identified. Here, to identify BIKE substrates, we conducted a barcode fusion genetics-yeast two-hybrid screen and retrieved publicly available data generated via affinity-purification mass spectrometry. We subsequently validated 19 of 47 putative BIKE interactors using mammalian cell–based protein–protein interaction assays. We found that CLINT1, a cargo-specific adapter implicated in bidirectional Golgi-to-endosome trafficking, emerged as a predominant hit in both screens. Our experiments indicated that BIKE catalyzes phosphorylation of a threonine 294 CLINT1 residue both in vitro and in cell culture. Our findings revealed that CLINT1 phosphorylation mediates its binding to the DENV nonstructural 3 protein and subsequently promotes DENV assembly and egress. Additionally, using live-cell imaging we revealed that CLINT1 cotraffics with DENV particles and is involved in mediating BIKE’s role in DENV infection. Finally, our data suggest that additional cellular BIKE interactors implicated in the host immune and stress responses and the ubiquitin proteasome system might also be candidate phosphorylation substrates of BIKE. In conclusion, these findings reveal cellular substrates and pathways regulated by the understudied Numb-associated kinase enzyme BIKE, a mechanism for CLINT1 regulation, and control of DENV infection via BIKE signaling, with potential implications for cell biology, virology, and host-targeted antiviral design. American Society for Biochemistry and Molecular Biology 2022-04-20 /pmc/articles/PMC9133654/ /pubmed/35452674 http://dx.doi.org/10.1016/j.jbc.2022.101956 Text en © 2022 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Article
Schor, Stanford
Pu, Szuyuan
Nicolaescu, Vlad
Azari, Siavash
Kõivomägi, Mardo
Karim, Marwah
Cassonnet, Patricia
Saul, Sirle
Neveu, Gregory
Yueh, Andrew
Demeret, Caroline
Skotheim, Jan M.
Jacob, Yves
Randall, Glenn
Einav, Shirit
The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection
title The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection
title_full The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection
title_fullStr The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection
title_full_unstemmed The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection
title_short The cargo adapter protein CLINT1 is phosphorylated by the Numb-associated kinase BIKE and mediates dengue virus infection
title_sort cargo adapter protein clint1 is phosphorylated by the numb-associated kinase bike and mediates dengue virus infection
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9133654/
https://www.ncbi.nlm.nih.gov/pubmed/35452674
http://dx.doi.org/10.1016/j.jbc.2022.101956
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