Your search keyword '"David C. Kochan"' showing total 3 results

1. Pathogenic variants in arteriopathy genes detected in a targeted sequencing study: Penetrance and 1-year outcomes after return of results

Author

Alborz Sherafati, Omar Elsekaily, Seyedmohammad Saadatagah, David C. Kochan, Christopher Lee, Georgia L. Wiesner, Cong Liu, Lisa Dellefave-Castillo, Bahram Namjou, Emma F. Perez, Zachary M. Salvati, John J. Connolly, Hakon Hakonarson, Marc S. Williams, Gail P. Jarvik, Wendy K. Chung, Elizabeth M. McNally, Teri A. Manolio, and Iftikhar J. Kullo

Subjects

Phenotype, Humans, Penetrance, Genomics, Genetics (clinical), Article

Abstract

PURPOSE: We estimated the penetrance of pathogenic/likely pathogenic (P/LP) variants in arteriopathy-related genes and assessed near-term outcomes following return of results. METHODS: Participants (N = 24,520) in phase III of the Electronic Medical Records and Genomics network underwent targeted sequencing of 68 actionable genes, including 9 genes associated with arterial aneurysmal diseases. Penetrance was estimated on the basis of the presence of relevant clinical traits. Outcomes occurring within 1 year of return of results included new diagnoses, referral to a specialist, new tests ordered, surveillance initiated, and new medications started. RESULTS: P/LP variants were present in 34 participants. The average penetrance across genes was 59%, ranging from 86% for FBN1 variants to 25% for SMAD3. Of 16 participants in whom results were returned, 1-year outcomes occurred in 63%. A new diagnosis was made in 44% of the participants, 56% were referred to a specialist, a new test was ordered in 44%, surveillance was initiated in 31%, and a new medication was started in 31%. CONCLUSION: Penetrance of P/LP variants in arteriopathy-related genes, identified in a large, targeted sequencing study, was variable and overall lower than that reported in clinical cohorts. Meaningful outcomes within the first year were noted in 63% of participants who received results.

Published

2022

2. Penetrance and outcomes at 1-year following return of actionable variants identified by genome sequencing

Author

Christopher, Lee, Omar, Elsekaily, David C, Kochan, Lubna, Alhalabi, Faizan, Faizee, Richard, Sharp, Noralane M, Lindor, and Iftikhar J, Kullo

Subjects

Genome, Phenotype, Humans, Penetrance, Genomics

Abstract

We estimated penetrance of actionable genetic variants and assessed near-term outcomes following return of results (RoR).Participants (n = 2,535) with hypercholesterolemia and/or colon polyps underwent targeted sequencing of 68 genes and 14 single-nucleotide variants. Penetrance was estimated based on presence of relevant traits in the electronic health record (EHR). Outcomes occurring within 1-year of RoR were ascertained by EHR review. Analyses were stratified by tier 1 and non-tier 1 disorders.Actionable findings were present in 122 individuals and results were disclosed to 98. The average penetrance for tier 1 disorder variants (67%; n = 58 individuals) was higher than in non-tier 1 variants (46.5%; n = 58 individuals). After excluding 45 individuals (decedents, nonresponders, known genetic diagnoses, mosaicism), ≥1 outcomes were noted in 83% of 77 participants following RoR; 78% had a process outcome (referral to a specialist, new testing, surveillance initiated); 68% had an intermediate outcome (new test finding or diagnosis); 19% had a clinical outcome (therapy modified, risk reduction surgery). Risk reduction surgery occurred more often in participants with tier 1 than those with non-tier 1 variants.Relevant phenotypic traits were observed in 57% whereas a clinical outcome occurred in 19% of participants with actionable genomic variants in the year following RoR.

Published

2020

3. Participant choices for return of genomic results in the eMERGE Network

Author

Julia Wynn, Nancy D. Leslie, Christin Hoell, David C. Kochan, John J. Connolly, Cynthia A. Prows, Luke V. Rasmussen, Keith Marsolo, Richard R. Sharp, Maureen E. Smith, Melanie F. Myers, Margaret Harr, Kathleen A. Leppig, Philip E. Lammers, Robert R. Freimuth, Ingrid A. Holm, Hakon Hakonarson, Wendy K. Chung, Sharon Aufox, and Iftikhar J. Kullo

Subjects

Adult, Genome, medicine.diagnostic_test, Adolescent, Process (engineering), Medical record, Applied psychology, Genomics, Preference, Article, Population Groups, Surveys and Questionnaires, medicine, Electronic Health Records, Humans, Psychology, Categorical variable, Genetics (clinical), Genetic testing

Abstract

PURPOSE: Secondary findings are typically offered in an all or none fashion when sequencing is used for clinical purposes. This study aims to describe the process of offering categorical and granular choices for results in a large research consortium. METHODS: Within the third phase of the electronic MEdical Records and GEnomics (eMERGE) Network, several sites implemented studies that allowed participants to choose the type of results they wanted to receive from a multigene sequencing panel. Sites were surveyed to capture the details of the implementation protocols and results of these choices. RESULTS: Across the ten eMERGE sites, 4664 participants including adolescents and adults were offered some type of choice. Categories of choices offered and methods for selecting categories varied. Most participants (94.5%) chose to learn all genetic results, while 5.5% chose subsets of results. Several sites allowed participants to change their choices at various time points, and 0.5% of participants made changes. CONCLUSION: Offering choices that include learning some results is important and should be a dynamic process to allow for changes in scientific knowledge, participant age group, and individual preference.

Published

2020