2018
DOI: 10.1016/j.semcdb.2017.08.056
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Alternative polyadenylation in the regulation and dysregulation of gene expression

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Cited by 54 publications
(52 citation statements)
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“…Alternative 39-end processing is critical for the regulation of gene expression because this action generates various mRNA isoforms harboring different cis-acting elements. As a consequence, different RNA-binding proteins or noncoding RNAs can be loaded onto the 39 UTR, thereby leading to different gene regulation outcomes (23)(24)(25)(26). Accordingly, the extended 39 UTR of poly(A) + RDH mRNAs should be subject to a mode of gene regulation different from that of canonical SL + RDH mRNAs.…”
Section: Discussionmentioning
confidence: 99%
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“…Alternative 39-end processing is critical for the regulation of gene expression because this action generates various mRNA isoforms harboring different cis-acting elements. As a consequence, different RNA-binding proteins or noncoding RNAs can be loaded onto the 39 UTR, thereby leading to different gene regulation outcomes (23)(24)(25)(26). Accordingly, the extended 39 UTR of poly(A) + RDH mRNAs should be subject to a mode of gene regulation different from that of canonical SL + RDH mRNAs.…”
Section: Discussionmentioning
confidence: 99%
“…Eukaryotic gene expression should be tightly regulated to adjust to cellular stresses. In particular, recent data reveal that alternative polyadenylation is affected by cellular stresses, such as cold or heat shock and UV irradiation (23)(24)(25)(26)(39)(40)(41)(42). It is also known that alternative polyadenylation is influenced by treatment with anisomycin, which inhibits the peptidyl transferase activity of a ribosome (43,44).…”
Section: Poly(a) + Rdh Mrnas Are Up-regulated Under Stress Conditionsmentioning
confidence: 99%
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“…Finally, we find a surprising degree of overlap between UPF1 targets and genes previously found to undergo 3'UTR "shortening" in cancer. Multiple lines of evidence suggest that preferential use of proximal pA sites in cancer is associated with increased expression of core cleavage and polyadenylation proteins (Turner et al, 2018), but our data indicate that nuclear control of 3'UTR isoform expression in cancer may be systematically augmented by NMD. These findings raise two possibilities that merit further investigation: first, NMD efficiency may contribute to 3'UTR isoform expression changes in cancer and second, APA may be in part used by cancer cells to evade NMD.…”
Section: Discussionmentioning
confidence: 55%
“…The PAT-seq approach identifies polyadenylation sites with exquisite sensitivity, which is confirmed by the high level of overlap with previously annotated positions of 3' UTRs in C. elegans (33) and our wild-type transcriptome (additional Fig 4a). A common idea is that the length of 3' UTR is correlated to the complexity of post-transcriptional regulation (34). Therefore, to ask if the 3' UTRs of GLD-2 target transcripts differ in any global parameters compared to those that are apparently not targeted, we first asked if there was a relationship between 3' UTR length and the change between wild-type and gld-2(0) adenylation state (additional Fig 4b).…”
Section: ' Utr Of Gld-2 Target Mrna Are Longer C-rich and Contain mentioning
confidence: 99%