The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells

Activation of CD4 T cells is a reaction to challenges such as microbial pathogens, cancer and toxins that defines adaptive immune responses. The roles of T cell receptor crosslinking, intracellular signaling, and transcription factor activation are well described, but the importance of post-transcri...

Descripción completa

Detalles Bibliográficos
Autores principales: Whisenant, Thomas C., Peralta, Eigen R., Aarreberg, Lauren D., Gao, Nina J., Head, Steven R., Ordoukhanian, Phillip, Williamson, Jamie R., Salomon, Daniel R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4671683/
https://www.ncbi.nlm.nih.gov/pubmed/26641092
http://dx.doi.org/10.1371/journal.pone.0144409
_version_ 1782404440652775424
author Whisenant, Thomas C.
Peralta, Eigen R.
Aarreberg, Lauren D.
Gao, Nina J.
Head, Steven R.
Ordoukhanian, Phillip
Williamson, Jamie R.
Salomon, Daniel R.
author_facet Whisenant, Thomas C.
Peralta, Eigen R.
Aarreberg, Lauren D.
Gao, Nina J.
Head, Steven R.
Ordoukhanian, Phillip
Williamson, Jamie R.
Salomon, Daniel R.
author_sort Whisenant, Thomas C.
collection PubMed
description Activation of CD4 T cells is a reaction to challenges such as microbial pathogens, cancer and toxins that defines adaptive immune responses. The roles of T cell receptor crosslinking, intracellular signaling, and transcription factor activation are well described, but the importance of post-transcriptional regulation by RNA-binding proteins (RBPs) has not been considered in depth. We describe a new model expanding and activating primary human CD4 T cells and applied this to characterizing activation-induced assembly of splicing factors centered on U2AF2. We immunoprecipitated U2AF2 to identify what mRNA transcripts were bound as a function of activation by TCR crosslinking and costimulation. In parallel, mass spectrometry revealed the proteins incorporated into the U2AF2-centered RNA/protein interactome. Molecules that retained interaction with the U2AF2 complex after RNAse treatment were designated as “central” interactome members (CIMs). Mass spectrometry also identified a second class of activation-induced proteins, “peripheral” interactome members (PIMs), that bound to the same transcripts but were not in physical association with U2AF2 or its partners. siRNA knockdown of two CIMs and two PIMs caused changes in activation marker expression, cytokine secretion, and gene expression that were unique to each protein and mapped to pathways associated with key aspects of T cell activation. While knocking down the PIM, SYNCRIP, impacts a limited but immunologically important set of U2AF2-bound transcripts, knockdown of U2AF1 significantly impairs assembly of the majority of protein and mRNA components in the activation-induced interactome. These results demonstrated that CIMs and PIMs, either directly or indirectly through RNA, assembled into activation-induced U2AF2 complexes and play roles in post-transcriptional regulation of genes related to cytokine secretion. These data suggest an additional layer of regulation mediated by the activation-induced assembly of RNA splicing interactomes that is important for understanding T cell activation.
format Online
Article
Text
id pubmed-4671683
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-46716832015-12-10 The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells Whisenant, Thomas C. Peralta, Eigen R. Aarreberg, Lauren D. Gao, Nina J. Head, Steven R. Ordoukhanian, Phillip Williamson, Jamie R. Salomon, Daniel R. PLoS One Research Article Activation of CD4 T cells is a reaction to challenges such as microbial pathogens, cancer and toxins that defines adaptive immune responses. The roles of T cell receptor crosslinking, intracellular signaling, and transcription factor activation are well described, but the importance of post-transcriptional regulation by RNA-binding proteins (RBPs) has not been considered in depth. We describe a new model expanding and activating primary human CD4 T cells and applied this to characterizing activation-induced assembly of splicing factors centered on U2AF2. We immunoprecipitated U2AF2 to identify what mRNA transcripts were bound as a function of activation by TCR crosslinking and costimulation. In parallel, mass spectrometry revealed the proteins incorporated into the U2AF2-centered RNA/protein interactome. Molecules that retained interaction with the U2AF2 complex after RNAse treatment were designated as “central” interactome members (CIMs). Mass spectrometry also identified a second class of activation-induced proteins, “peripheral” interactome members (PIMs), that bound to the same transcripts but were not in physical association with U2AF2 or its partners. siRNA knockdown of two CIMs and two PIMs caused changes in activation marker expression, cytokine secretion, and gene expression that were unique to each protein and mapped to pathways associated with key aspects of T cell activation. While knocking down the PIM, SYNCRIP, impacts a limited but immunologically important set of U2AF2-bound transcripts, knockdown of U2AF1 significantly impairs assembly of the majority of protein and mRNA components in the activation-induced interactome. These results demonstrated that CIMs and PIMs, either directly or indirectly through RNA, assembled into activation-induced U2AF2 complexes and play roles in post-transcriptional regulation of genes related to cytokine secretion. These data suggest an additional layer of regulation mediated by the activation-induced assembly of RNA splicing interactomes that is important for understanding T cell activation. Public Library of Science 2015-12-07 /pmc/articles/PMC4671683/ /pubmed/26641092 http://dx.doi.org/10.1371/journal.pone.0144409 Text en © 2015 Whisenant 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
Whisenant, Thomas C.
Peralta, Eigen R.
Aarreberg, Lauren D.
Gao, Nina J.
Head, Steven R.
Ordoukhanian, Phillip
Williamson, Jamie R.
Salomon, Daniel R.
The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells
title The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells
title_full The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells
title_fullStr The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells
title_full_unstemmed The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells
title_short The Activation-Induced Assembly of an RNA/Protein Interactome Centered on the Splicing Factor U2AF2 Regulates Gene Expression in Human CD4 T Cells
title_sort activation-induced assembly of an rna/protein interactome centered on the splicing factor u2af2 regulates gene expression in human cd4 t cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4671683/
https://www.ncbi.nlm.nih.gov/pubmed/26641092
http://dx.doi.org/10.1371/journal.pone.0144409
work_keys_str_mv AT whisenantthomasc theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT peraltaeigenr theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT aarreberglaurend theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT gaoninaj theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT headstevenr theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT ordoukhanianphillip theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT williamsonjamier theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT salomondanielr theactivationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT whisenantthomasc activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT peraltaeigenr activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT aarreberglaurend activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT gaoninaj activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT headstevenr activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT ordoukhanianphillip activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT williamsonjamier activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells
AT salomondanielr activationinducedassemblyofanrnaproteininteractomecenteredonthesplicingfactoru2af2regulatesgeneexpressioninhumancd4tcells

Ejemplares similares