A Novel Role for Nucleolin in Splice Site Selection

Shefer, Kinneret; Boulos, Ayub; Gotea, Valer; Chaim, Yair Ben; Sperling, Joseph; Elnitski, Laura; Sperling, Ruth

doi:10.1101/2020.12.02.402354

Cited by 1 publication

(1 citation statement)

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“…NCL in the nuclear speckles colocalizes with SC35 (as we also observe in our study), and is reported to interact with the pre-catalytic spliceosome complex and regulate AS of fibronectin ( 80 ). NCL is also known to play a major role in splice site selection ( 81 ). qRT-PCR performed to detect exon inclusion events for selected transcripts established the role of rG4s in AS.…”

Section: Discussionmentioning

confidence: 99%

Retracted: Alternative splicing modulation mediated by G-quadruplex structures in MALAT1 lncRNA

Ghosh

Pandey

Ansari

et al. 2021

Nucleic Acids Research

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MALAT1, an abundant lncRNA specifically localized to nuclear speckles, regulates alternative-splicing (AS). The molecular basis of its role in AS remains poorly understood. Here, we report three conserved, thermodynamically stable, parallel RNA-G-quadruplexes (rG4s) present in the 3′ region of MALAT1 which regulates this function. Using rG4 domain-specific RNA-pull-down followed by mass-spectrometry, RNA-immuno-precipitation, and imaging, we demonstrate the rG4 dependent localization of Nucleolin (NCL) and Nucleophosmin (NPM) to nuclear speckles. Specific G-to-A mutations that abolish rG4 structures, result in the localization loss of both the proteins from speckles. Functionally, disruption of rG4 in MALAT1 phenocopies NCL knockdown resulting in altered pre-mRNA splicing of endogenous genes. These results reveal a central role of rG4s within the 3′ region of MALAT1 orchestrating AS.

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Section: Discussionmentioning

confidence: 99%