Clinical and laboratory genetic counselor attitudes on the reporting of variants of uncertain significance for multigene cancer panels

Emmeline Y Chang; Ilana Solomon; Julie O Culver; Nicholas Gorman; Jacob G Comeaux; Caryn Lerman; Emily A Quinn; Tali Ekstein

doi:10.1002/jgc4.1680

Clinical and laboratory genetic counselor attitudes on the reporting of variants of uncertain significance for multigene cancer panels

J Genet Couns. 2023 Jun;32(3):706-716. doi: 10.1002/jgc4.1680. Epub 2023 Feb 6.

Authors

Emmeline Y Chang^{1

2}, Ilana Solomon³, Julie O Culver¹, Nicholas Gorman², Jacob G Comeaux¹, Caryn Lerman¹, Emily A Quinn², Tali Ekstein⁴

Affiliations

¹ USC Norris Comprehensive Cancer Center, University of Southern California, Los Angeles, California, USA.
² Department of Human Genetics and Genetic Counseling, Keck Graduate Institute, Claremont, California, USA.
³ Center for Precision Medicine, City of Hope, Duarte, California, USA.
⁴ Clinical Consultation Services, Invitae, San Francisco, California, USA.

PMID: 36747331
DOI: 10.1002/jgc4.1680

Abstract

Research suggests variants of uncertain significance (VUSs) present a variety of challenges for genetic counselors (GCs), nongenetics clinicians, and patients. Multigene cancer panels reveal more VUSs than single gene testing as a result of the increase in the number of genes being tested. This study surveyed 87 clinical cancer GCs involved with direct patient care and 19 laboratory GCs who provide guidance to clinicians regarding genetic test results about their attitudes on various options for the reporting of VUSs by laboratories for broad multigene cancer panels. Independent samples t-tests were utilized to compare the two groups. Based on a six-point Likert-type scale (1 = Strongly Disagree to 6 = Strongly Agree), clinical cancer GCs (M = 5.4; SD = 0.8) and laboratory GCs (M = 5.2; SD = 0.9) agreed overall that VUSs should be reported (p = 0.44; Cohen's d = 0.21). When asked about specific reporting options, both clinical cancer GCs (M = 1.9; SD = 1.1) and laboratory GCs (M = 2.1; SD = 1.4) disagreed that VUSs should be reported only for genes related to the indication for testing (p = 0.50; Cohen's d = 0.17). Overall, most GCs felt clinicians should not choose whether VUSs should be reported on genetic test results, with clinical cancer GCs (M = 1.9; SD = 1.3) feeling more strongly against it than laboratory GCs (M = 3.1; SD = 1.4; p = 0.002; Cohen's d = 0.88). Generally, GCs were more in favor of VUSs not being reported for population-based screening, with laboratory GCs (M = 4.7; SD = 0.8) agreeing more with that practice than clinical cancer GCs (M = 3.7; SD = 1.4; p = 0.001; Cohen's d = 0.80). Both clinical cancer GCs (M = 4.1; SD = 1.2) and laboratory GCs (M = 3.9; SD = 1.2) agreed additional guidelines on how to approach VUSs in clinical practice should be developed (p = 0.54; Cohen's d = 0.17). While most GCs supported the reporting of VUSs overall, our analyses suggest clinical cancer and laboratory GCs may have different attitudes toward specific VUS-related reporting options. Further research is needed to elucidate GC preferences to help inform best practices for the reporting of VUSs. The development of additional standardized guidelines on how to approach VUSs would further support clinical practice.

Keywords: attitudes; cancer; genetic counselors; genetic testing; laboratory; laboratory report; multigene panel; variant of uncertain significance.

MeSH terms

Attitude
Counselors*
Genetic Predisposition to Disease
Genetic Testing / methods
Humans
Laboratories
Neoplasms*