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Open AccessJournal ArticleDOI

Ubiquitously transcribed genes use alternative polyadenylation to achieve tissue-specific expression

TLDR
This work developed a sequencing method called 3'-seq to quantitatively map the 3' ends of the transcriptome of diverse human tissues and isogenic transformation systems and found that cell type-specific gene expression is accomplished by two complementary programs.
Abstract
More than half of human genes use alternative cleavage and polyadenylation (ApA) to generate mRNA transcripts that differ in the lengths of their 3' untranslated regions (UTRs), thus altering the post-transcriptional fate of the message and likely the protein output. The extent of 3' UTR variation across tissues and the functional role of ApA remain poorly understood. We developed a sequencing method called 3'-seq to quantitatively map the 3' ends of the transcriptome of diverse human tissues and isogenic transformation systems. We found that cell type-specific gene expression is accomplished by two complementary programs. Tissue-restricted genes tend to have single 3' UTRs, whereas a majority of ubiquitously transcribed genes generate multiple 3' UTRs. During transformation and differentiation, single-UTR genes change their mRNA abundance levels, while multi-UTR genes mostly change 3' UTR isoform ratios to achieve tissue specificity. However, both regulation programs target genes that function in the same pathways and processes that characterize the new cell type. Instead of finding global shifts in 3' UTR length during transformation and differentiation, we identify tissue-specific groups of multi-UTR genes that change their 3' UTR ratios; these changes in 3' UTR length are largely independent from changes in mRNA abundance. Finally, tissue-specific usage of ApA sites appears to be a mechanism for changing the landscape targetable by ubiquitously expressed microRNAs.

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Citations
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Posted ContentDOI

Transcription is ubiquitously terminated in thousands of bidirectional termination zones in yeast

Gang Zhen, +1 more
- 03 Nov 2022 - 
TL;DR: In this paper , a fine-scale view of transcription termination in eukaryotic genomes is presented. But the authors focus on the UAUAUAUA motifs, which are ubiquitously used as termination sites for both coding and non-coding genes.
Posted ContentDOI

Discovery of global regulators of 3′ untranslated region processing in cancers with KAPAC

TL;DR: PAQR and KAPAC methods enable the identification of regulatory factors that shape 3′ UTR processing and the characterization of their binding position-dependent activity in physiological and pathological cell states, including human malignancies.
Posted ContentDOI

Alternative polyadenylation regulates acetyl-CoA carboxylase function in peanut

TL;DR: In this paper , the authors performed long-read single-molecule sequencing of mRNA from peanut seeds, which revealed that more than half of all peanut genes have more than two polyadenylation sites (PASs) with more PASs in older developing seeds, indicating that the PAS is highly tissue specific and plays an important role in peanut seed maturation.
Journal ArticleDOI

REPAC: analysis of alternative polyadenylation from RNA-sequencing data

TL;DR: In this paper , a framework for the analysis of alternative polyadenylation (APA) from RNA-sequencing data is presented, and the landscape of APA caused by activation of B cells is investigated.
DissertationDOI

Characterizing Alternative Polyadenylation in Male Germ Cells Using Poly(A)-seq

Holly Tran
TL;DR: Investigation of male germ cell-specific transcripts associated with alternative polyadenylation will lead to an improved understanding of molecular regulation involved in spermatogenesis and factors that cause male infertility, and suggests that PolyA-seq is a reliable method for transcriptome characterization.
References
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Journal ArticleDOI

MicroRNAs: Genomics, Biogenesis, Mechanism, and Function

TL;DR: Although they escaped notice until relatively recently, miRNAs comprise one of the more abundant classes of gene regulatory molecules in multicellular organisms and likely influence the output of many protein-coding genes.
Journal ArticleDOI

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Simon Anders, +1 more
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Journal ArticleDOI

MicroRNA expression profiles classify human cancers

TL;DR: A new, bead-based flow cytometric miRNA expression profiling method is used to present a systematic expression analysis of 217 mammalian miRNAs from 334 samples, including multiple human cancers, and finds the miRNA profiles are surprisingly informative, reflecting the developmental lineage and differentiation state of the tumours.
Journal ArticleDOI

A mammalian microRNA expression atlas based on small RNA library sequencing.

TL;DR: A relatively small set of miRNAs, many of which are ubiquitously expressed, account for most of the differences in miRNA profiles between cell lineages and tissues.
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