Literature DB >> 20220758

Understanding mechanisms underlying human gene expression variation with RNA sequencing.

Joseph K Pickrell1, John C Marioni, Athma A Pai, Jacob F Degner, Barbara E Engelhardt, Everlyne Nkadori, Jean-Baptiste Veyrieras, Matthew Stephens, Yoav Gilad, Jonathan K Pritchard.   

Abstract

Understanding the genetic mechanisms underlying natural variation in gene expression is a central goal of both medical and evolutionary genetics, and studies of expression quantitative trait loci (eQTLs) have become an important tool for achieving this goal. Although all eQTL studies so far have assayed messenger RNA levels using expression microarrays, recent advances in RNA sequencing enable the analysis of transcript variation at unprecedented resolution. We sequenced RNA from 69 lymphoblastoid cell lines derived from unrelated Nigerian individuals that have been extensively genotyped by the International HapMap Project. By pooling data from all individuals, we generated a map of the transcriptional landscape of these cells, identifying extensive use of unannotated untranslated regions and more than 100 new putative protein-coding exons. Using the genotypes from the HapMap project, we identified more than a thousand genes at which genetic variation influences overall expression levels or splicing. We demonstrate that eQTLs near genes generally act by a mechanism involving allele-specific expression, and that variation that influences the inclusion of an exon is enriched within and near the consensus splice sites. Our results illustrate the power of high-throughput sequencing for the joint analysis of variation in transcription, splicing and allele-specific expression across individuals.

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Year:  2010        PMID: 20220758      PMCID: PMC3089435          DOI: 10.1038/nature08872

Source DB:  PubMed          Journal:  Nature        ISSN: 0028-0836            Impact factor:   49.962


  29 in total

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9.  High-resolution mapping of expression-QTLs yields insight into human gene regulation.

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2.  Estimation of alternative splicing variability in human populations.

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6.  Rapid and robust resampling-based multiple-testing correction with application in a genome-wide expression quantitative trait loci study.

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Review 7.  Using chromatin marks to interpret and localize genetic associations to complex human traits and diseases.

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Review 10.  Determining causality and consequence of expression quantitative trait loci.

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