IDEAS home Printed from https://ideas.repec.org/a/nat/nature/v581y2020i7809d10.1038_s41586-020-2329-2.html
   My bibliography  Save this article

Transcript expression-aware annotation improves rare variant interpretation

Author

Listed:
  • Beryl B. Cummings

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital
    Harvard Medical School)

  • Konrad J. Karczewski

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital)

  • Jack A. Kosmicki

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital
    Harvard Medical School)

  • Eleanor G. Seaby

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital
    University Hospital Southampton)

  • Nicholas A. Watts

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital)

  • Moriel Singer-Berk

    (Broad Institute of MIT and Harvard)

  • Jonathan M. Mudge

    (Wellcome Genome Campus)

  • Juha Karjalainen

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital
    Broad Institute of MIT and Harvard)

  • F. Kyle Satterstrom

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital
    Broad Institute of MIT and Harvard)

  • Anne H. O’Donnell-Luria

    (Broad Institute of MIT and Harvard
    Boston Children’s Hospital
    Harvard Medical School)

  • Timothy Poterba

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital
    Broad Institute of MIT and Harvard)

  • Cotton Seed

    (Massachusetts General Hospital
    Broad Institute of MIT and Harvard)

  • Matthew Solomonson

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital)

  • Jessica Alföldi

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital)

  • Mark J. Daly

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital)

  • Daniel G. MacArthur

    (Broad Institute of MIT and Harvard
    Massachusetts General Hospital
    Garvan Institute of Medical Research, and UNSW Sydney
    Murdoch Children’s Research Institute)

Abstract

The acceleration of DNA sequencing in samples from patients and population studies has resulted in extensive catalogues of human genetic variation, but the interpretation of rare genetic variants remains problematic. A notable example of this challenge is the existence of disruptive variants in dosage-sensitive disease genes, even in apparently healthy individuals. Here, by manual curation of putative loss-of-function (pLoF) variants in haploinsufficient disease genes in the Genome Aggregation Database (gnomAD)1, we show that one explanation for this paradox involves alternative splicing of mRNA, which allows exons of a gene to be expressed at varying levels across different cell types. Currently, no existing annotation tool systematically incorporates information about exon expression into the interpretation of variants. We develop a transcript-level annotation metric known as the ‘proportion expressed across transcripts’, which quantifies isoform expression for variants. We calculate this metric using 11,706 tissue samples from the Genotype Tissue Expression (GTEx) project2 and show that it can differentiate between weakly and highly evolutionarily conserved exons, a proxy for functional importance. We demonstrate that expression-based annotation selectively filters 22.8% of falsely annotated pLoF variants found in haploinsufficient disease genes in gnomAD, while removing less than 4% of high-confidence pathogenic variants in the same genes. Finally, we apply our expression filter to the analysis of de novo variants in patients with autism spectrum disorder and intellectual disability or developmental disorders to show that pLoF variants in weakly expressed regions have similar effect sizes to those of synonymous variants, whereas pLoF variants in highly expressed exons are most strongly enriched among cases. Our annotation is fast, flexible and generalizable, making it possible for any variant file to be annotated with any isoform expression dataset, and will be valuable for the genetic diagnosis of rare diseases, the analysis of rare variant burden in complex disorders, and the curation and prioritization of variants in recall-by-genotype studies.

Suggested Citation

  • Beryl B. Cummings & Konrad J. Karczewski & Jack A. Kosmicki & Eleanor G. Seaby & Nicholas A. Watts & Moriel Singer-Berk & Jonathan M. Mudge & Juha Karjalainen & F. Kyle Satterstrom & Anne H. O’Donnell, 2020. "Transcript expression-aware annotation improves rare variant interpretation," Nature, Nature, vol. 581(7809), pages 452-458, May.
    • Handle: RePEc:nat:nature:v:581:y:2020:i:7809:d:10.1038_s41586-020-2329-2
    DOI: 10.1038/s41586-020-2329-2
    as

    Download full text from publisher

    File URL: https://www.nature.com/articles/s41586-020-2329-2
    File Function: Abstract
    Download Restriction: Access to the full text of the articles in this series is restricted.
    File URL: https://libkey.io/10.1038/s41586-020-2329-2?utm_source=ideas
    LibKey link: if access is restricted and if your library uses this service, LibKey will redirect you to where you can use your library subscription to access this item
    ---><---

    As the access to this document is restricted, you may want to search for a different version of it.

    Citations

    Citations are extracted by the CitEc Project, subscribe to its RSS feed for this item.
    as


    Cited by:

    1. Scott D. Findlay & Lindsay Romo & Christopher B. Burge, 2024. "Quantifying negative selection in human 3ʹ UTRs uncovers constrained targets of RNA-binding proteins," Nature Communications, Nature, vol. 15(1), pages 1-15, December.
    2. Matt C. Danzi & Maike F. Dohrn & Sarah Fazal & Danique Beijer & Adriana P. Rebelo & Vivian Cintra & Stephan Züchner, 2023. "Deep structured learning for variant prioritization in Mendelian diseases," Nature Communications, Nature, vol. 14(1), pages 1-16, December.
    3. Mischan Vali-Pour & Solip Park & Jose Espinosa-Carrasco & Daniel Ortiz-Martínez & Ben Lehner & Fran Supek, 2022. "The impact of rare germline variants on human somatic mutation processes," Nature Communications, Nature, vol. 13(1), pages 1-21, December.

    More about this item

    Statistics

    Access and download statistics

    Corrections

    All material on this site has been provided by the respective publishers and authors. You can help correct errors and omissions. When requesting a correction, please mention this item's handle: RePEc:nat:nature:v:581:y:2020:i:7809:d:10.1038_s41586-020-2329-2. See general information about how to correct material in RePEc.

    If you have authored this item and are not yet registered with RePEc, we encourage you to do it here. This allows to link your profile to this item. It also allows you to accept potential citations to this item that we are uncertain about.

    We have no bibliographic references for this item. You can help adding them by using this form .

    If you know of missing items citing this one, you can help us creating those links by adding the relevant references in the same way as above, for each refering item. If you are a registered author of this item, you may also want to check the "citations" tab in your RePEc Author Service profile, as there may be some citations waiting for confirmation.

    For technical questions regarding this item, or to correct its authors, title, abstract, bibliographic or download information, contact: Sonal Shukla or Springer Nature Abstracting and Indexing (email available below). General contact details of provider: http://www.nature.com .

    Please note that corrections may take a couple of weeks to filter through the various RePEc services.

    IDEAS is a RePEc service. RePEc uses bibliographic data supplied by the respective publishers.