Reciprocal regulation of hnRNP C and CELF2 through translation and transcription tunes splicing activity in T cells

RNA binding proteins (RBPs) frequently regulate the expression of other RBPs in mammalian cells. Such cross-regulation has been proposed to be important to control networks of coordinated gene expression; however, much remains to be understood about how such networks of cross-regulation are establis...

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Veröffentlicht in:	Nucleic acids research 2020-06, Vol.48 (10), p.5710-5719
Hauptverfasser:	Mallory, Michael J, McClory, Sean P, Chatrikhi, Rakesh, Gazzara, Matthew R, Ontiveros, Robert J, Lynch, Kristen W
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Schlagworte:	RNA and RNA-protein complexes
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creator	Mallory, Michael J McClory, Sean P Chatrikhi, Rakesh Gazzara, Matthew R Ontiveros, Robert J Lynch, Kristen W
description	RNA binding proteins (RBPs) frequently regulate the expression of other RBPs in mammalian cells. Such cross-regulation has been proposed to be important to control networks of coordinated gene expression; however, much remains to be understood about how such networks of cross-regulation are established and what the functional consequence is of coordinated or reciprocal expression of RBPs. Here we demonstrate that the RBPs CELF2 and hnRNP C regulate the expression of each other, such that depletion of one results in reduced expression of the other. Specifically, we show that loss of hnRNP C reduces the transcription of CELF2 mRNA, while loss of CELF2 results in decreased efficiency of hnRNP C translation. We further demonstrate that this reciprocal regulation serves to fine tune the splicing patterns of many downstream target genes. Together, this work reveals new activities of hnRNP C and CELF2, provides insight into a previously unrecognized gene regulatory network, and demonstrates how cross-regulation of RBPs functions to shape the cellular transcriptome.
doi_str_mv	10.1093/nar/gkaa295
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subjects	RNA and RNA-protein complexes
title	Reciprocal regulation of hnRNP C and CELF2 through translation and transcription tunes splicing activity in T cells
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