Reporting Incidental Findings in Genomic Scale Clinical Sequencing—A Clinical Laboratory Perspective

Hegde, Madhuri; Bale, Sherri J.; Bayrak-Toydemir, Pınar; Gibson, Jane; Jeng, Linda Jo Bone; Joseph, Loren; Laser, Jordan; Lubin, Ira M.; Miller, Christine; Ross, Lainie Friedman; Rothberg, Paul G.; Tanner, Alice K.; Vitazka, Patrik; Mao, Rong

doi:10.1016/j.jmoldx.2014.10.004

Cited by 53 publications

(58 citation statements)

References 32 publications

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“…Reporting of predictive secondary variants to the patients is a highly debated subject (Shahmirzadi et al 2014), because of potential false positives (Kohane et al 2006; Biesecker 2013; Hegde et al 2015). Indeed, we found 22 candidate variants in the ACMG approved 56 gene set, and is likely nearly all of these are sequence errors.…”

Section: Discussionmentioning

confidence: 99%

CAGI4 SickKids clinical genomes challenge: A pipeline for identifying pathogenic variants

et al. 2017

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Compared with earlier more restricted sequencing technologies, identification of rare disease variants using whole genome sequence has the possibility of finding all causative variants, but issues of data quality and an overwhelming level of background variants complicate the analysis. The CAGI4 SickKids clinical genome challenge provided an opportunity to assess the landscape of variants found in a difficult set of 25 unsolved rare disease cases. To address the challenge, we developed a three-stage pipeline, first carefully analyzing data quality, then classifying high quality gene specific variants into seven categories, and finally examining each candidate variant for compatibility with the often complex phenotypes of these patients for final prioritization. Variants consistent with the phenotypes were found in 24 out of the 25 cases, and in a number of these, there are prioritized variants in multiple genes. Data quality analysis suggests that some of the selected variants are likely incorrect calls, complicating interpretation. The data providers followed up on three suggested variants with Sanger sequencing, and in one case a prioritized variant was confirmed as likely causative by the referring physician, providing a diagnosis in a previously intractable case.

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Section: Discussionmentioning

confidence: 99%

CAGI4 SickKids clinical genomes challenge: A pipeline for identifying pathogenic variants

et al. 2017

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“…107,109 For secondary findings revealed in germline testing, the ACMG recommends disclosure of positive germline results for 53 genes, approximately half of which are associated with cancer predisposition susceptibility genes that will likely be on somatic testing panels. 108 Disclosure is recommended even when the germline is only being evaluated as part of a tumor/normal study.…”

Section: Germline Variants Identified During Cancer Testingmentioning

confidence: 99%

Standards and Guidelines for the Interpretation and Reporting of Sequence Variants in Cancer

Datto

Duncavage

et al. 2017

The Journal of Molecular Diagnostics

1,330

954

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Widespread clinical laboratory implementation of next-generation sequencingebased cancer testing has highlighted the importance and potential benefits of standardizing the interpretation and reporting of molecular results among laboratories. A multidisciplinary working group tasked to assess the current status of next-generation sequencingebased cancer testing and establish standardized consensus classification, annotation, interpretation, and reporting conventions for somatic sequence variants was

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“…Instead, the AMP group endorsed “opt-in or opt-out…in the precounseling session.” 31 The group elaborated, [P]ersons undergoing WES or WGS should have the opportunity to opt-in or opt-out of receiving a report that documents variants that are not relevant to the initial reason for testing…. Most patients will likely opt-in, given the opportunity to receive additional information that could be used to improve their health.…”

Section: Continuing Problems With Acmg Policymentioning

confidence: 99%

The Continuing Evolution of Ethical Standards for Genomic Sequencing in Clinical Care: Restoring Patient Choice

Wolf¹

2017

J. Law. Med. Ethics

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Developing ethical standards for clinical use of large-scale genome and exome sequencing has proven challenging, in part due to the inevitability of incidental or secondary findings. Policy of the American College of Medical Genetics and Genomics (ACMG) has evolved but remains problematic. In 2013, ACMG issued policy recommending mandatory analysis of 56 extra genes whenever sequencing was ordered for any indication, in order to ascertain positive findings in pathogenic and actionable genes. Widespread objection yielded a 2014 amendment allowing patients to opt-out from analysis of the extra genes. In 2015, ACMG published the amended policy, providing that patients could opt out of the full set of extra genes, but not a subset. In 2016, ACMG enlarged the set and indicated planned expansion of the roster of extra genes to include pharmacogenetic findings. ACMG policy does not protect the respect for patient choice that prevails in other domains of clinical medicine, where informed consent allows patients to opt in to desired testing. By creating an expanding domain of genomic testing that will be routinely conducted unless patients reject the entire set of extra tests, ACMG creates an exceptional domain clinical practice that is not supported by ethics or science.

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Reporting Incidental Findings in Genomic Scale Clinical Sequencing—A Clinical Laboratory Perspective

Cited by 53 publications

References 32 publications

CAGI4 SickKids clinical genomes challenge: A pipeline for identifying pathogenic variants

CAGI4 SickKids clinical genomes challenge: A pipeline for identifying pathogenic variants

Standards and Guidelines for the Interpretation and Reporting of Sequence Variants in Cancer

The Continuing Evolution of Ethical Standards for Genomic Sequencing in Clinical Care: Restoring Patient Choice

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