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Paraspeckle-independent co-transcriptional regulation of nuclear microRNA biogenesis by SFPQ

Caroline Thivierge, Maxime Bellefeuille, Sarah-Slim Diwan, Boris J.A. Dyakov, Rania Leventis, Gabrielle Perron, Hamed S. Najafabadi, Simon‐Pierre Gravel, Anne‐Claude Gingras, Thomas F. Duchaîne

2024Cell Reports12 citationsDOIOpen Access PDF

Abstract

MicroRNAs (miRNAs) play crucial roles in physiological functions and disease, but the regulation of their nuclear biogenesis remains poorly understood. Here, BioID on Drosha, the catalytic subunit of the microprocessor complex, reveals its proximity to splicing factor proline- and glutamine (Q)-rich (SFPQ), a multifunctional RNA-binding protein (RBP) involved in forming paraspeckle nuclear condensates. SFPQ depletion impacts both primary and mature miRNA expression, while other paraspeckle proteins (PSPs) or the paraspeckle scaffolding RNA NEAT1 do not, indicating a paraspeckle-independent role. Comprehensive transcriptomic analyses show that SFPQ loss broadly affects RNAs and miRNA host gene (HG) expression, influencing both their transcription and the stability of their products. Notably, SFPQ protects the oncogenic miR-17∼92 polycistron from degradation by the nuclear exosome targeting (NEXT)-exosome complex and is tightly linked with its overexpression across a broad variety of cancers. Our findings reveal a dual role for SFPQ in regulating miRNA HG transcription and stability, as well as its significance in cancers.

Topics & Concepts

DroshaRNA-binding proteinBiologymicroRNACell biologyGene silencingRNA splicingExosomeSplicing factorRegulation of gene expressionRNA interferenceRNAGeneticsGeneMicrovesiclesRNA Research and SplicingRNA modifications and cancerRNA regulation and disease