2020
DOI: 10.7554/elife.59186
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Single molecule poly(A) tail-seq shows LARP4 opposes deadenylation throughout mRNA lifespan with most impact on short tails

Abstract: La-related protein 4 (LARP4) directly binds both poly(A) and poly(A)-binding protein (PABP). LARP4 was shown to promote poly(A) tail (PAT) lengthening and stabilization of individual mRNAs presumably by protection from deadenylation (Mattijssen et al., 2017). We developed a nucleotide resolution transcriptome-wide, single molecule SM-PAT-seq method. This revealed LARP4 effects on a wide range of PAT lengths for human mRNAs and mouse mRNAs from LARP4 knockout (KO) and control cells. LARP4 effects are clear on l… Show more

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Cited by 25 publications
(30 citation statements)
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“…From our WGCNA, we identified candidate GWAS-related genes LARP4 and PIP4K2C as respective hub genes for the plum4 and lightsteelblue modules. In other model systems, LARP4 has been implicated in mRNA stabilization [ 44 ]. Consistent with this, the plum4 module was enriched for numerous regulatory processes including posttranscriptional regulation of gene expression.…”
Section: Discussionmentioning
confidence: 99%
“…From our WGCNA, we identified candidate GWAS-related genes LARP4 and PIP4K2C as respective hub genes for the plum4 and lightsteelblue modules. In other model systems, LARP4 has been implicated in mRNA stabilization [ 44 ]. Consistent with this, the plum4 module was enriched for numerous regulatory processes including posttranscriptional regulation of gene expression.…”
Section: Discussionmentioning
confidence: 99%
“…EEF2 (eukaryotic elongation factor 2) is a GTP binding translation elongation factor, which plays an essential role in translation by promoting GTP dependent translocation of the ribosome (66). LARP4 binds to the poly-A tract of mRNA, associates with the 40S ribosomal subunit as well as polysomes and plays a role in translation regulation by preventing deadenylation at poly-A tail (67)(68)(69). Presence of these factors in the HEV IRESl RNA-associated protein complex suggests their potential role(s) in regulating the HEV IRESl-mediated translation.…”
Section: Discussionmentioning
confidence: 99%
“…(Houseley et al 2006) Even so, the transcriptome-wide analyses of poly(A)-tail length started only when the TAIL-seq (Chang et al 2014) and PAL-seq (Subtelny et al 2014) methods broke through the homopolymer base-calling technical limits. In recent years the Nanopore technology (Garalde et al 2018) and PacBio system (Legnini et al 2019;Liu et al 2019;Mattijssen et al 2020) also proved to overcome homopolymer-reading barriers. However, all such methods for the high-quality homopolymer reading must rely on an elaborate sequencer-dependent library-preparing plan that inevitably introduces biases in sequencing.…”
Section: Discussionmentioning
confidence: 99%
“…(Chang et al 2014; Lim et al 2016; Lima et al 2017) An internal standard and calibration curve method in PAL-seq was utilized to estimate poly(A)-tail length. (Subtelny et al 2014; Eisen et al 2020) Further advancements in long-read sequencing by Nanopore(Garalde et al 2018; Nicholson-Shaw et al 2022) and PacBio(Legnini et al 2019; Liu et al 2019; Mattijssen et al 2020; Long et al 2021) also handled homopolymeric sequences through repeatedly correcting reading-errors. All these methods have indeed expanded our understanding of the dynamic nature of the mRNA poly(A) tail.…”
Section: Introductionmentioning
confidence: 99%