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Nucleoporin TPR is an integral component of the TREX-2 mRNA export pathway

Vasilisa Aksenova, Alexandra Smith, Hangnoh Lee, Prasanna Bhat, Caroline Esnault, Shane Chen, James Iben, Ross Kaufhold, Ka Chun Yau, Carlos Echeverría, Beatriz M. A. Fontoura, Alexei Arnaoutov, Mary Dasso

2020Nature Communications139 citationsDOIOpen Access PDF

Abstract

Nuclear pore complexes (NPCs) are important for cellular functions beyond nucleocytoplasmic trafficking, including genome organization and gene expression. This multi-faceted nature and the slow turnover of NPC components complicates investigations of how individual nucleoporins act in these diverse processes. To address this question, we apply an Auxin-Induced Degron (AID) system to distinguish roles of basket nucleoporins NUP153, NUP50 and TPR. Acute depletion of TPR causes rapid and pronounced changes in transcriptomic profiles. These changes are dissimilar to shifts observed after loss of NUP153 or NUP50, but closely related to changes caused by depletion of mRNA export receptor NXF1 or the GANP subunit of the TRanscription-EXport-2 (TREX-2) mRNA export complex. Moreover, TPR depletion disrupts association of TREX-2 subunits (GANP, PCID2, ENY2) to NPCs and results in abnormal RNA transcription and export. Our findings demonstrate a unique and pivotal role of TPR in gene expression through TREX-2- and/or NXF1-dependent mRNA turnover.

Topics & Concepts

NucleoporinNuclear poreMessenger RNACell biologyNuclear export signalProtein subunitTranscriptomeTranscription (linguistics)Transcription factorBiologyNuclear transportGene expressionGeneChemistryCell nucleusNucleusGeneticsPhilosophyLinguisticsNuclear Structure and FunctionRNA Research and SplicingRNA regulation and disease
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