Cross-species analysis of viral nucleic acid interacting proteins identifies TAOKs as innate immune regulators

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作者
Friederike L. Pennemann
Assel Mussabekova
Christian Urban
Alexey Stukalov
Line Lykke Andersen
Vincent Grass
Teresa Maria Lavacca
Cathleen Holze
Lila Oubraham
Yasmine Benamrouche
Enrico Girardi
Rasha E. Boulos
Rune Hartmann
Giulio Superti-Furga
Matthias Habjan
Jean-Luc Imler
Carine Meignin
Andreas Pichlmair
机构
[1] Technical University of Munich,Computer Science and Mathematics Department, School of Arts and Science
[2] School of Medicine,Center for Physiology and Pharmacology
[3] Institute of Virology,undefined
[4] Université de Strasbourg,undefined
[5] CNRS UPR9022,undefined
[6] Institut de Biologie Moléculaire et Cellulaire,undefined
[7] Innate Immunity Laboratory,undefined
[8] Max-Planck Institute of Biochemistry,undefined
[9] CeMM - Center for Molecular Medicine of the Austrian Academy of Sciences,undefined
[10] Lebanese American University,undefined
[11] Aarhus University,undefined
[12] Department of Molecular Biology and Genetics - Structural Biology,undefined
[13] Medical University of Vienna,undefined
[14] German Center for Infection Research (DZIF),undefined
[15] Munich partner site,undefined
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摘要
The cell intrinsic antiviral response of multicellular organisms developed over millions of years and critically relies on the ability to sense and eliminate viral nucleic acids. Here we use an affinity proteomics approach in evolutionary distant species (human, mouse and fly) to identify proteins that are conserved in their ability to associate with diverse viral nucleic acids. This approach shows a core of orthologous proteins targeting viral genetic material and species-specific interactions. Functional characterization of the influence of 181 candidates on replication of 6 distinct viruses in human cells and flies identifies 128 nucleic acid binding proteins with an impact on virus growth. We identify the family of TAO kinases (TAOK1, −2 and −3) as dsRNA-interacting antiviral proteins and show their requirement for type-I interferon induction. Depletion of TAO kinases in mammals or flies leads to an impaired response to virus infection characterized by a reduced induction of interferon stimulated genes in mammals and impaired expression of srg1 and diedel in flies. Overall, our study shows a larger set of proteins able to mediate the interaction between viral genetic material and host factors than anticipated so far, attesting to the ancestral roots of innate immunity and to the lineage-specific pressures exerted by viruses.
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