Weber et al. 2022 (PRJNA744147)

General Details

Title Monitoring the 5′UTR landscape reveals isoform switches to drive translational efficiencies in cancer
Organism
Number of Samples 1
Release Date 2021/07/06 00:00
Sequencing Types
Protocol Details

Study Links

Repository Details

SRA SRP327136
ENA SRP327136
GEO GSE179525
BioProject PRJNA744147

Publication

Title
Authors Weber R,Ghoshdastider U,Spies D,Duré C,Valdivia-Francia F,Forny M,Ormiston M,Renz PF,Taborsky D,Yigit M,Bernasconi M,Yamahachi H,Sendoel A
Journal Oncogene
Publication Date 2023 Feb
Abstract Transcriptional and translational control are key determinants of gene expression, however, to what extent these two processes can be collectively coordinated is still poorly understood. Here, we use Nanopore long-read sequencing and cap analysis of gene expression (CAGE-seq) to document the landscape of 5' and 3' untranslated region (UTR) isoforms and transcription start sites of epidermal stem cells, wild-type keratinocytes and squamous cell carcinomas. Focusing on squamous cell carcinomas, we show that a small cohort of genes with alternative 5'UTR isoforms exhibit overall increased translational efficiencies and are enriched in ribosomal proteins and splicing factors. By combining polysome fractionations and CAGE-seq, we further characterize two of these UTR isoform genes with identical coding sequences and demonstrate that the underlying transcription start site heterogeneity frequently results in 5' terminal oligopyrimidine (TOP) and pyrimidine-rich translational element (PRTE) motif switches to drive mTORC1-dependent translation of the mRNA. Genome-wide, we show that highly translated squamous cell carcinoma transcripts switch towards increased use of 5'TOP and PRTE motifs, have generally shorter 5'UTRs and expose decreased RNA secondary structures. Notably, we found that the two 5'TOP motif-containing, but not the TOP-less, RPL21 transcript isoforms strongly correlated with overall survival in human head and neck squamous cell carcinoma patients. Our findings warrant isoform-specific analyses in human cancer datasets and suggest that switching between 5'UTR isoforms is an elegant and simple way to alter protein synthesis rates, set their sensitivity to the mTORC1-dependent nutrient-sensing pathway and direct the translational potential of an mRNA by the precise 5'UTR sequence. © 2022. The Author(s).
PMC PMC9957725
PMID 36550360
DOI
Run Accession Study Accession Scientific Name Cell Line Library Type Treatment GWIPS-viz Trips-Viz Reads BAM BigWig (F) BigWig (R)
SRR15049345 PRJNA744147 Mus musculus Primary keratinocytes from P0 back skin Ribo-Seq
Run Accession Study Accession Scientific Name Cell Line Library Type Treatment GWIPS-viz Trips-Viz Reads BAM BigWig (F) BigWig (R)

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