Clinical challenges in interpreting multiple pathogenic mutations in single patients

Christa Slaught; Elizabeth G. Berry; Lindsay Bacik; Alison H. Skalet; George Anadiotis; Therese Tuohy; Sancy A. Leachman

doi:10.1186/s13053-021-00172-3

Hereditary Cancer in Clinical Practice (Feb 2021)

Clinical challenges in interpreting multiple pathogenic mutations in single patients

Christa Slaught,
Elizabeth G. Berry,
Lindsay Bacik,
Alison H. Skalet,
George Anadiotis,
Therese Tuohy,
Sancy A. Leachman

Affiliations

Christa Slaught: Department of Dermatology, Oregon Health & Science University
Elizabeth G. Berry: Department of Dermatology, Oregon Health & Science University
Lindsay Bacik: Department of Dermatology, Penn State Health
Alison H. Skalet: Department of Dermatology, Oregon Health & Science University
George Anadiotis: Legacy Cancer Institute, Cancer Genetics Services, Legacy Health Systems
Therese Tuohy: Legacy Cancer Institute, Cancer Genetics Services, Legacy Health Systems
Sancy A. Leachman: Department of Dermatology, Oregon Health & Science University

DOI: https://doi.org/10.1186/s13053-021-00172-3
Journal volume & issue: Vol. 19, no. 1
pp. 1 – 11

Abstract

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Abstract Background In the past two decades, genetic testing for cancer risk assessment has entered mainstream clinical practice due to the availability of low-cost panels of multiple cancer-associated genes. However, the clinical value of multiple-gene panels for cancer susceptibility is not well established, especially in cases where panel testing identifies more than one pathogenic variant. The risk for specific malignancies as a result of a mutated gene is complex and likely influenced by superimposed modifier variants and/or environmental effects. Recent data suggests that the combination of multiple pathogenic variants may be fewer than reported by chance, suggesting that some mutation combinations may be detrimental. Management of patients with “incidentally” discovered mutations can be particularly challenging, especially when established guidelines call for radical procedures (e.g. total gastrectomy in CDH1) in patients and families without a classic clinical history concerning for that cancer predisposition syndrome. Case presentation We present two cases, one of an individual and one of a family, with multiple pathogenic mutations detected by multi-gene panel testing to highlight challenges practitioners face in counseling patients about pathogenic variants and determining preventive and therapeutic interventions. Conclusions Ongoing investigation is needed to improve our understanding of inherited susceptibility to disease in general and cancer predisposition syndromes, as this information has the potential to lead to the development of more precise and patient-specific counseling and surveillance strategies. The real-world adoption of new or improved technologies into clinical practice frequently requires medical decision-making in the absence of established understanding of gene-gene interactions. In the meantime, practitioners must be prepared to apply a rationale based on currently available knowledge to clinical decision-making. Current practice is evolving to rely heavily on clinical concordance with personal and family history in making specific therapeutic decisions.

Published in Hereditary Cancer in Clinical Practice

ISSN: 1897-4287 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens; Science: Biology (General): Genetics
Website: https://hccpjournal.biomedcentral.com/

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