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. 2017 Jul;19(7):787-795.
doi: 10.1038/gim.2016.191. Epub 2017 Jan 26.

Assigning clinical meaning to somatic and germ-line whole-exome sequencing data in a prospective cancer precision medicine study

Arezou A Ghazani  1   2   3 Nelly M Oliver  1   2 Joseph P St Pierre  2 Andrea Garofalo  3 Irene R Rainville  2   4 Elaine Hiller  2   4 Daniel J Treacy  1   2 Vanesa Rojas-Rudilla  5 Sam Wood  2 Elizabeth Bair  2 Michael Parello  2 Franklin Huang  2   3 Marios Giannakis  2   3 Frederick H Wilson  2   3 Elizabeth H Stover  2   3 Steven M Corsello  2   3 Tom Nguyen  2 Huma Q Rana  2   4 Alanna J Church  6 Carol Lowenstein  2 Carrie Cibulskis  3 Ali Amin-Mansour  3 Jennifer Heng  2 Lauren Brais  2 Abigail Santos  2 Patrick Bauer  2 Amanda Waldron  2 Peter Lo  2 Megan Gorman  2 Christine A Lydon  2 Marisa Welch  2 Philip McNamara  2 Stacey Gabriel  3 Lynette M Sholl  5 Neal I Lindeman  5 Judy E Garber  2   4 Steven Joffe  7 Eliezer M Van Allen  1   2   3 Stacy W Gray  2 Pasi A Ja Nne  2 Levi A Garraway  1   2   3 Nikhil Wagle  1   2   3
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Free article

Assigning clinical meaning to somatic and germ-line whole-exome sequencing data in a prospective cancer precision medicine study

Arezou A Ghazani et al. Genet Med. 2017 Jul.
Free article

Abstract

Purpose: Implementing cancer precision medicine in the clinic requires assessing the therapeutic relevance of genomic alterations. A main challenge is the systematic interpretation of whole-exome sequencing (WES) data for clinical care.

Methods: One hundred sixty-five adults with metastatic colorectal and lung adenocarcinomas were prospectively enrolled in the CanSeq study. WES was performed on DNA extracted from formalin-fixed paraffin-embedded tumor biopsy samples and matched blood samples. Somatic and germ-line alterations were ranked according to therapeutic or clinical relevance. Results were interpreted using an integrated somatic and germ-line framework and returned in accordance with patient preferences.

Results: At the time of this analysis, WES had been performed and results returned to the clinical team for 165 participants. Of 768 curated somatic alterations, only 31% were associated with clinical evidence and 69% with preclinical or inferential evidence. Of 806 curated germ-line variants, 5% were clinically relevant and 56% were classified as variants of unknown significance. The variant review and decision-making processes were effective when the process was changed from that of a Molecular Tumor Board to a protocol-based approach.

Conclusion: The development of novel interpretive and decision-support tools that draw from scientific and clinical evidence will be crucial for the success of cancer precision medicine in WES studies.Genet Med advance online publication 26 January 2017.

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References

    1. Cell. 2013 Mar 28;153(1):17-37 - PubMed
    1. Nat Med. 2014 Jun;20(6):682-8 - PubMed
    1. J Clin Oncol. 2013 May 20;31(15):1825-33 - PubMed
    1. JAMA Oncol. 2016 Jan;2(1):104-11 - PubMed
    1. Sci Transl Med. 2015 Apr 15;7(283):283ra53 - PubMed

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