Your search keyword '"Erin Thorpe"' showing total 17 results

1. Clinical genome sequencing in patients with suspected rare genetic disease in Peru

Author

Jeny Bazalar-Montoya, Mario Cornejo-Olivas, Milagros M. Duenas-Roque, Nelson Purizaca-Rosillo, Richard S. Rodriguez, Karina Milla-Neyra, Carlos A. De La Torre-Hernandez, Elison Sarapura-Castro, Carolina I. Galarreta Aima, Gioconda Manassero-Morales, Giulliana Chávez-Pasco, Luis Celis-García, Jorge E. La Serna-Infantes, Illumina Laboratory Services Bioinformatics, Software, Interpretation and Customer Support, Evgenii Chekalin, Erin Thorpe, and Ryan J. Taft

Subjects

Medicine, Genetics, QH426-470

Abstract

Abstract There is limited access to molecular genetic testing in most low- and middle-income countries. The iHope program provides clinical genome sequencing (cGS) to underserved individuals with signs or symptoms of rare genetic diseases and limited or no access to molecular genetic testing. Here we describe the performance and impact of cGS in 247 patients from three clinics in Peru. Although most patients had at least one genetic test prior to cGS (70.9%), the most frequent was karyotyping (53.4%). The diagnostic yield of cGS was 54.3%, with candidate variants reported in an additional 22.3% of patients. Clinical GS results impacted clinician diagnostic evaluation in 85.0% and genetic counseling in 72.1% of cases. Changes in management were reported in 71.3%, inclusive of referrals (64.7%), therapeutics (26.3%), laboratory or physiological testing (25.5%), imaging (19%), and palliative care (17.4%), suggesting that increased availability of genomic testing in Peru would enable improved patient management.

Published

2024

2. P368: Novel mutation in ZIC3 in a Peruvian family with variable phenotype VACTERL-H association

Author

Giulliana Chávez-Pasco, Jeny Bazalar-Montoya, Cecilia Bonilla Suarez, Krista Bluske, Samuel Strom, Alka Malhotra, Becky Milewski, Erin Thorpe, Ryan Taft, and Gioconda Manassero-Morales

Subjects

Genetics, QH426-470, Medicine

Published

2024

3. P412: A heterozygous 287 kb deletion of the X chromosome in a Peruvian girl with dystrophinopathy

Author

Jeny Bazalar-Montoya, Richard Rodriguez, Giulliana Chávez-Pasco, Peggy Martínez-Esteban, Revathi Rajkumar, Akanchha Kesari, Carolyn Brown, Erin Thorpe, Ryan Taft, and Gioconda Manassero-Morales

Subjects

Genetics, QH426-470, Medicine

Published

2024

4. P624: Performance and impact of clinical genome sequencing in patients with suspected rare genetic diseases in Peru

Author

Erin Thorpe, Milagros Duenas-Roque, Mario Cornejo-Olivas, Jeny Bazalar-Montoya, Nelson Purizaca-Rosillo, Richard Rodriguez, Karina Milla-Neyra, Carlos De La Torre-Hernandez, Elison Sarapura-Castro, Carolina Galarreta Aima, Gioconda Manassero-Morales, Giulliana Chávez-Pasco, Luis Celis-García, Jorge La Serna, and Ryan Taft

Subjects

Genetics, QH426-470, Medicine

Published

2024

5. Reactive gene curation to support interpretation and reporting of a clinical genome test for rare disease: Experience from over 1,000 cases

Author

Amanda R. Clause, Julie P. Taylor, Revathi Rajkumar, Krista Bluske, Maren Bennett, Laura M. Amendola, David R. Bentley, Ryan J. Taft, Denise L. Perry, Alison J. Coffey, Carolyn Brown, Matthew P. Brown, Amanda Buchanan, Brendan Burns, Nicole J. Burns, Anjana Chandrasekhar, Aditi Chawla, Katie Golden-Grant, Akanchha Kesari, Alka Malhotra, Becky Milewski, Samin A. Sajan, Zinayida Schlachetzki, Sarah Schmidt, Brittany Thomas, and Erin Thorpe

Subjects

rare disease, RUGD, gene curation, gene-disease relationship, GDR, genome sequencing, Genetics, QH426-470, Internal medicine, RC31-1245

Abstract

Summary: Current standards in clinical genetics recognize the need to establish the validity of gene-disease relationships as a first step in the interpretation of sequence variants. We describe our experience incorporating the ClinGen Gene-Disease Clinical Validity framework in our interpretation and reporting workflow for a clinical genome sequencing (cGS) test for individuals with rare and undiagnosed genetic diseases. This “reactive” gene curation is completed upon identification of candidate variants during active case analysis and within the test turn-around time by focusing on the most impactful evidence and taking advantage of the broad applicability of the framework to cover a wide range of disease areas. We demonstrate that reactive gene curation can be successfully implemented in support of cGS in a clinical laboratory environment, enabling robust clinical decision making and allowing all variants to be fully and appropriately considered and their clinical significance confidently interpreted.

Published

2023

6. O38: The impact of whole genome sequencing in a diverse global population of genetic disease patients

Author

Ryan Taft, Erin Thorpe, John Belmont, Taylor Williams, Chad Shaw, Jason Button, Julia Ortega, Keisha Robinson, Marilyn Jones, Diane Masser-Frye, Donald Basel, Chester Brown, Keith Vaux, Aime Lumaka, Fabio Sirchia, Milagros Dueñas Roque, Mario Cornejo-Olivas, Jeny Bazalar-Montoya, Nora Urraca, Alejandra Salguero, Samuel Wiafe, Romina Foster-Bonds, Erin Royer, Michelle Gallas, Pilar Magoulas, Adeline Vanderver, Marwan Shinawi, Alan Taylor, Kristen Fishler, Duncan Henry, Daria Salyakina, Kate Gibson, Melissa Lah, Alka Malhotra, James Avecilla, Andrew Warren, Denise Perry, and Max Arseneault

Subjects

Genetics, QH426-470, Medicine

Published

2023

7. P572: Detecting short tandem repeat expansions: Three-year experience with clinical whole genome sequencing (cWGS) for a rare and undiagnosed population

Author

Brittany Thomas, Akanchha Kesari, Aime Lumaka, Mario Cornejo-Olivas, David Ward, Parul Jayakar, Donald Basel, Marilyn Jones, Erin Thorpe, Denise Perry, and Ryan Taft

Subjects

Genetics, QH426-470, Medicine

Published

2023

8. X-linked neonatal-onset epileptic encephalopathy associated with a gain-of-function variant p.R660T in GRIA3.

Author

Jia-Hui Sun, Jiang Chen, Fernando Eduardo Ayala Valenzuela, Carolyn Brown, Diane Masser-Frye, Marilyn Jones, Leslie Patron Romero, Berardo Rinaldi, Wenhui Laura Li, Qing-Qing Li, Dan Wu, Benedicte Gerard, Erin Thorpe, Allan Bayat, and Yun Stone Shi

Subjects

Genetics, QH426-470

Abstract

The X-linked GRIA3 gene encodes the GLUA3 subunit of AMPA-type glutamate receptors. Pathogenic variants in this gene were previously reported in neurodevelopmental diseases, mostly in male patients but rarely in females. Here we report a de novo pathogenic missense variant in GRIA3 (c.1979G>C; p. R660T) identified in a 1-year-old female patient with severe epilepsy and global developmental delay. When exogenously expressed in human embryonic kidney (HEK) cells, GLUA3_R660T showed slower desensitization and deactivation kinetics compared to wildtype (wt) GLUA3 receptors. Substantial non-desensitized currents were observed with the mutant but not for wt GLUA3 with prolonged exposure to glutamate. When co-expressed with GLUA2, the decay kinetics were similarly slowed in GLUA2/A3_R660T with non-desensitized steady state currents. In cultured cerebellar granule neurons, miniature excitatory postsynaptic currents (mEPSCs) were significantly slower in R660T transfected cells than those expressing wt GLUA3. When overexpressed in hippocampal CA1 neurons by in utero electroporation, the evoked EPSCs and mEPSCs were slower in neurons expressing R660T mutant compared to those expressing wt GLUA3. Therefore our study provides functional evidence that a gain of function (GoF) variant in GRIA3 may cause epileptic encephalopathy and global developmental delay in a female subject by enhancing synaptic transmission.

Published

2021

9. The landscape of reported VUS in multi-gene panel and genomic testing: Time for a change

Author

Heidi L Rehm, Joseph T Alaimo, Swaroop Aradhya, Pinar Bayrak-Toydemir, Hunter Best, Rhonda Brandon, Jillian G Buchan, Elizabeth C Chao, Elaine Chen, Jacob Clifford, Ana S Cohen, Laura K Conlin, Soma Das, Kyle W Davis, Daniela del Gaudio, Florencia Del Viso, Christina DiVincenzo, Marcia Eisenberg, Lucia Guidugli, Monia B Hammer, Steven M Harrison, Kathryn E Hatchell, Lindsay Havens Dyer, Lily U Hoang, James M Holt, Vaidehi Jobanputra, Izabela D Karbassi, Hutton M Kearney, Melissa A Kelly, Jacob M Kelly, Michelle L Kluge, Timothy Komala, Paul Kruszka, Lynette Lau, Matthew S Lebo, Christian R Marshall, Dianalee McKnight, Kirsty McWalter, Yan Meng, Narasimhan Nagan, Christian S Neckelmann, Nir Neerman, Zhiyv Niu, Vitoria K Paolillo, Sarah A Paolucci, Denise Perry, Tina Pesaran, Kelly Radtke, Kristen J Rasmussen, Kyle Retterer, Carol J Saunders, Elizabeth Spiteri, Christine M Stanley, Anna Szuto, Ryan J Taft, Isabelle Thiffault, Brittany C Thomas, Amanda Thomas-Wilson, Erin Thorpe, Timothy J Tidwell, Meghan C Towne, and Hana Zouk

Abstract

Variants of uncertain significance (VUS) are a common result of diagnostic genetic testing and can be difficult to manage with potential misinterpretation and downstream costs, including time investment by clinicians. We investigated the rate of VUS reported on diagnostic testing via multi-gene panels (MGPs) and exome and genome sequencing (ES/GS) to measure the magnitude of uncertain results and explore ways to reduce their potentially detrimental impact. We collected data from over 1.5 million genetic tests from 19 clinical laboratories across the United States and Canada from during 2020-2021. We found a lower rate of inconclusive results due to VUS on ES/GS tests compared to MGPs (22.5% vs. 32.6%; p

Published

2022

10. A clinical laboratory's experience using GeneMatcher—Building stronger gene–disease relationships

Author

Julie P. Taylor, Alka Malhotra, Nicole J. Burns, Amanda R. Clause, Carolyn M. Brown, Brendan T. Burns, Anjana Chandrasekhar, Zinayida Schlachetzki, Maren Bennett, Erin Thorpe, Ryan J. Taft, Denise L. Perry, and Alison J. Coffey

Subjects

Whole Genome Sequencing, Genetics, High-Throughput Nucleotide Sequencing, Humans, Laboratories, Clinical, Genetics (clinical)

Abstract

The use of whole-genome sequencing (WGS) has accelerated the pace of gene discovery and highlighted the need for open and collaborative data sharing in the search for novel disease genes and variants. GeneMatcher (GM) is designed to facilitate connections between researchers, clinicians, health-care providers, and others to help in the identification of additional patients with variants in the same candidate disease genes. The Illumina Clinical Services Laboratory offers a WGS test for patients with suspected rare and undiagnosed genetic disease and regularly submits potential candidate genes to GM to strengthen gene-disease relationships. We describe our experience with GM, including criteria for evaluation of candidate genes, and our workflow for the submission and review process. We have made 69 submissions, 36 of which are currently active. Ten percent of submissions have resulted in publications, with an additional 14 submissions part of ongoing collaborations and expected to result in a publication.

Published

2022

11. X-linked neonatal-onset epileptic encephalopathy associated with a gain-of-function variant p.R660T in GRIA3

Author

Qing Qing Li, Diane Masser-Frye, Wenhui Laura Li, Berardo Rinaldi, Carolyn Brown, Marilyn C. Jones, Dan Wu, Erin Thorpe, Leslie Patrón Romero, Jiang Chen, Bénédicte Gérard, Allan Bayat, Fernando Eduardo Ayala Valenzuela, Yun Stone Shi, Jia Hui Sun, and zhang, wei

Subjects

Models, Molecular, Cancer Research, Protein Conformation, Gene Expression, Sequence Homology, QH426-470, Neurodegenerative, Biochemistry, Hippocampus, Infantile, Spasms, Mice, 0302 clinical medicine, Animal Cells, Models, Cerebellum, Receptors, AMPA, Medicine and Health Sciences, 2.1 Biological and endogenous factors, GRIA3, Aetiology, Receptor, Child, Genetics (clinical), Neurons, Mice, Inbred ICR, 0303 health sciences, Glutamate receptor, Brain, Neurochemistry, Neurotransmitters, Genomics, Transfection, Inbred ICR, Amino Acid, Neurology, Child, Preschool, Gain of Function Mutation, Neurological, Excitatory postsynaptic potential, Cell lines, Female, Cellular Types, Glutamate, Anatomy, Biological cultures, Spasms, Infantile, Research Article, medicine.medical_specialty, Primary Cell Culture, Neurotransmission, Biology, Research and Analysis Methods, 03 medical and health sciences, Fluctuation Analysis, Internal medicine, Computational Techniques, medicine, Genetics, Animals, Humans, Receptors, AMPA, Amino Acid Sequence, Molecular Biology Techniques, Preschool, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Epilepsy, Sequence Homology, Amino Acid, HEK 293 cells, Egg Proteins, Wild type, Neurosciences, Biology and Life Sciences, Membrane Proteins, Molecular, Cell Biology, Brain Disorders, Endocrinology, HEK293 Cells, Cellular Neuroscience, biology.protein, Sequence Alignment, 030217 neurology & neurosurgery, Neuroscience, Developmental Biology

Abstract

The X-linked GRIA3 gene encodes the GLUA3 subunit of AMPA-type glutamate receptors. Pathogenic variants in this gene were previously reported in neurodevelopmental diseases, mostly in male patients but rarely in females. Here we report a de novo pathogenic missense variant in GRIA3 (c.1979G>C; p. R660T) identified in a 1-year-old female patient with severe epilepsy and global developmental delay. When exogenously expressed in human embryonic kidney (HEK) cells, GLUA3_R660T showed slower desensitization and deactivation kinetics compared to wildtype (wt) GLUA3 receptors. Substantial non-desensitized currents were observed with the mutant but not for wt GLUA3 with prolonged exposure to glutamate. When co-expressed with GLUA2, the decay kinetics were similarly slowed in GLUA2/A3_R660T with non-desensitized steady state currents. In cultured cerebellar granule neurons, miniature excitatory postsynaptic currents (mEPSCs) were significantly slower in R660T transfected cells than those expressing wt GLUA3. When overexpressed in hippocampal CA1 neurons by in utero electroporation, the evoked EPSCs and mEPSCs were slower in neurons expressing R660T mutant compared to those expressing wt GLUA3. Therefore our study provides functional evidence that a gain of function (GoF) variant in GRIA3 may cause epileptic encephalopathy and global developmental delay in a female subject by enhancing synaptic transmission., Author summary Glutamate is the excitatory neurotransmitter in brain, abnormality of which causes excitotoxicity and diseases. Here we identified a pathogenic missense variant in GRIA3 gene in a female patient with severe epilepsy and global developmental delay. The X-linked GRIA3 gene encodes GLUA3, a subunit of glutamate receptors. Through electrophysiological analysis of the mutant GLUA3 in a cell line and mouse neurons, we found this mutant makes strengthened glutamate receptors. This study thus indicates that the variant causes epileptic encephalopathy and global developmental delay by enhancing glutamate signaling in brain.

Published

2021

12. Copy-number variants in clinical genome sequencing: deployment and interpretation for rare and undiagnosed disease

Author

Alison J. Coffey, Alka Malhotra, Bryan R. Lajoie, Egor Dolzhenko, Denise L. Perry, Alicia Scocchia, R. Tanner Hagelstrom, Amirah Khouzam, Ryan J. Taft, Vani Rajan, Tina Hambuch, Stephen Tanner, Natasa Dzidic, Shimul Chowdhury, Andrew M. Gross, Trilochan Sahoo, Eric Roller, Subramanian S. Ajay, Erin Thorpe, Nicole J. Burns, Karine Hovanes, Sergii Ivakhno, David R. Bentley, Julia McEachern, Michael A. Eberle, Carolyn Brown, John W Belmont, Aditi Chawla, and Krista Bluske

Subjects

Male, 0301 basic medicine, Adolescent, DNA Copy Number Variations, Microarray, whole genome sequencing (WGS), Computational biology, Disease, 030105 genetics & heredity, Biology, Undiagnosed Diseases, Article, DNA sequencing, Cohort Studies, Young Adult, 03 medical and health sciences, Rare Diseases, medicine, Humans, Genetic Testing, Copy-number variation, Child, Genetics (clinical), Whole Genome Sequencing, Genome, Human, Breakpoint, Chromosome Mapping, Infant, Genomics, medicine.disease, Uniparental disomy, rare and undiagnosed disease, copy number variation (CNV), 030104 developmental biology, Child, Preschool, structural variation (SV), Female, DNA microarray, Trisomy, microarray

Abstract

Purpose Current diagnostic testing for genetic disorders involves serial use of specialized assays spanning multiple technologies. In principle, genome sequencing (GS) can detect all genomic pathogenic variant types on a single platform. Here we evaluate copy-number variant (CNV) calling as part of a clinically accredited GS test. Methods We performed analytical validation of CNV calling on 17 reference samples, compared the sensitivity of GS-based variants with those from a clinical microarray, and set a bound on precision using orthogonal technologies. We developed a protocol for family-based analysis of GS-based CNV calls, and deployed this across a clinical cohort of 79 rare and undiagnosed cases. Results We found that CNV calls from GS are at least as sensitive as those from microarrays, while only creating a modest increase in the number of variants interpreted (~10 CNVs per case). We identified clinically significant CNVs in 15% of the first 79 cases analyzed, all of which were confirmed by an orthogonal approach. The pipeline also enabled discovery of a uniparental disomy (UPD) and a 50% mosaic trisomy 14. Directed analysis of select CNVs enabled breakpoint level resolution of genomic rearrangements and phasing of de novo CNVs. Conclusion Robust identification of CNVs by GS is possible within a clinical testing environment.

Published

2019

13. A framework designed to improve the evaluation and reporting of incidental findings in clinical genomic tests

Author

Denise L. Perry, Ryan J. Taft, Anjana Chandrasekhar, R. Tanner Hagelstrom, Alison J. Coffey, Erin Thorpe, and Carolyn Brown

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Molecular Biology, Biochemistry

Published

2021

14. Clinical whole genome sequencing as a first-tier test at a resource-limited dysmorphology clinic in Mexico

Author

Marilyn C. Jones, Carolina I. Galarreta, Denise L. Perry, Miguel Del Campo, Reporting Team, Vani Rajan, Diane Masser-Frye, Kristen Wigby, David R. Bentley, Ryan J. Taft, Alicia Scocchia, Subramanian S. Ajay, Keisha D Robinson, Julia McEachern, Andrew M. Gross, Erin Thorpe, Icsl Interpretation, and John W Belmont

Subjects

0301 basic medicine, Proband, Pediatrics, medicine.medical_specialty, lcsh:QH426-470, MEDLINE, lcsh:Medicine, Disease, Article, 03 medical and health sciences, 0302 clinical medicine, Clinical Research, medicine, Genetics, Copy-number variation, Genetic Testing, Medical diagnosis, Molecular Biology, Genetics (clinical), Whole genome sequencing, Pediatric, screening and diagnosis, business.industry, lcsh:R, ICSL Interpretation and Reporting Team, Human Genome, medicine.disease, Test (assessment), 4.1 Discovery and preclinical testing of markers and technologies, lcsh:Genetics, Detection, 030104 developmental biology, Good Health and Well Being, 030220 oncology & carcinogenesis, Trisomy, business, 4.2 Evaluation of markers and technologies

Abstract

Patients with rare, undiagnosed, or genetic disease (RUGD) often undergo years of serial testing, commonly referred to as the “diagnostic odyssey”. Patients in resource-limited areas face even greater challenges—a definitive diagnosis may never be reached due to difficulties in gaining access to clinicians, appropriate specialists, and diagnostic testing. Here, we report on a collaboration of the Illumina iHope Program with the Foundation for the Children of the Californias and Hospital Infantil de Las Californias, to enable deployment of clinical whole genome sequencing (cWGS) as first-tier test in a resource-limited dysmorphology clinic in northern Mexico. A total of 60 probands who were followed for a suspected genetic diagnosis and clinically unresolved after expert examination were tested with cWGS, and the ordering clinicians completed a semi-structured survey to investigate change in clinical management resulting from cWGS findings. Clinically significant genomic findings were identified in 68.3% (n = 41) of probands. No recurrent molecular diagnoses were observed. Copy number variants or gross chromosomal abnormalities accounted for 48.8% (n = 20) of the diagnosed cases, including a mosaic trisomy and suspected derivative chromosomes. A qualitative assessment of clinical management revealed 48.8% (n = 20) of those diagnosed had a change in clinical course based on their cWGS results, despite resource limitations. These data suggest that a cWGS first-tier testing approach can benefit patients with suspected genetic disorders., Pediatrics: Philanthropic clinical whole-genome sequencing program helps children in Mexico Whole-genome sequencing (WGS) provides a valuable first-tier diagnostic test at pediatric clinics in resource-limited parts of the world, according to a study of children with suspected genetic disease treated in northern Mexico. A team led by Marilyn Jones from the Rady Children’s Hospital and Ryan Taft from Illumina Inc., both in San Diego, California, USA, describe a collaboration with a volunteer-led clinic in Tijuana, Mexico, where they offered genome sequencing for children with suspected genetic conditions—philanthropically through the iHope Program. Among the 60 families that participated, the clinical laboratory team identified genomic variants with diagnostic relevance in 41 (68%) cases. The genomic information contributed to changes in clinical management for 20 of these children, demonstrating the impact of WGS in places where patients generally don’t have access to medical specialists or other sophisticated molecular tests.

Published

2019

15. Multiple molecular diagnoses in individual patients identified through whole genome sequencing

Author

Alka Malhotra, Julia L Ortega, Ryan J. Taft, Erin Thorpe, John W. Belmont, Diane Masser-Frye, Erin Royer, Denise L. Perry, Marilyn C. Jones, Laura Davis-Keppen, and Lisa Ohden

Subjects

Whole genome sequencing, Endocrinology, Endocrinology, Diabetes and Metabolism, Genetics, Computational biology, Biology, Molecular Biology, Biochemistry

Published

2021

16. Copy number variants in clinical WGS: deployment and interpretation for rare and undiagnosed disease

Author

Krista Bluske, Carolyn Brown, Trilochan Sahoo, Alison J. Coffey, Andrew M. Gross, Michael A. Eberle, Rajan, Amirah Khouzam, Ryan J. Taft, Egor Dolzhenko, Natasa Dzidic, Erin Thorpe, Alka Malhotra, Denise L. Perry, Aditi Chawla, Julia McEachern, John W Belmont, Eric Roller, Nicole J. Burns, Sergii Ivakhno, David R. Bentley, Karine Hovanes, Bryan R. Lajoie, Tina Hambuch, Stephen Tanner, Subramanian S. Ajay, Alicia Scocchia, R. Tanner Hagelstrom, and Shimul Chowdhury

Subjects

Whole genome sequencing, Microarray, Clinical cohort, Computer science, medicine, Copy-number variation, Disease, Computational biology, DNA microarray, Trisomy, medicine.disease, Uniparental disomy

Abstract

PurposeCurrent diagnostic testing for genetic disorders involves serial use of specialized assays spanning multiple technologies. In principle, whole genome sequencing (WGS) has the potential to detect all genomic mutation types on a single platform and workflow. Here we sought to evaluate copy number variant (CNV) calling as part of a clinically accredited WGS test.MethodsUsing a depth-based copy number caller we performed analytical validation of CNV calling on a reference panel of 17 samples, compared the sensitivity of WGS-based variants to those from a clinical microarray, and set a bound on precision using orthogonal technologies. We developed a protocol for family-based analysis, annotation, filtering, visualization of WGS based CNV calls, and deployed this across a clinical cohort of 79 rare and undiagnosed cases.ResultsWe found that CNV calls from WGS are at least as sensitive as those from microarrays, while only creating a modest increase in the number of variants interpreted (~10 CNVs per case). We identified clinically significant CNVs in 15% of the first 79 cases analyzed. This pipeline also enabled identification of cases of uniparental disomy (UPD) and a 50% mosaic trisomy 14. Directed analysis of some CNVs enabled break-point level resolution of genomic rearrangements and phasing ofde-novoCNVs.ConclusionRobust identification of CNVs by WGS is possible within a clinical testing environment, and further developments will bring improvements in resolution of smaller and more complex CNVs.

Published

2018

17. Experiences of Genetic Counselors Practicing in Rural Areas

Author

MaryAnn Campion, Margaret M. Emmet, Quinn Stein, and Erin Thorpe

Subjects

0301 basic medicine, Adult, Male, Rural Population, medicine.medical_specialty, Referral, Service delivery framework, media_common.quotation_subject, Genetic counseling, education, Genetic Counseling, 030105 genetics & heredity, 03 medical and health sciences, Nursing, Surveys and Questionnaires, Medicine, Humans, Genetics (clinical), Qualitative Research, media_common, business.industry, Public health, Awareness, Outreach, Counselors, Female, Personal experience, Rural Health Services, Rural area, business, Autonomy

Abstract

In-person genetic counseling clinics in rural areas are likely to improve access to genetic counseling in underserved regions, but studies have not previously examined how these clinics function or described the experience of practicing in a rural setting. The present mixed-methods study explored the professional experiences of clinical genetic counselors who practice in rural areas, including the benefits and challenges of practicing in these settings and the counselors’ motivations for doing so. The authors surveyed 20 genetic counselors who self-reported working in rural areas and conducted interviews with six individuals whose workplaces were confirmed as rural per RUCA code. Major obstacles to the provision of genetics services in rural areas included travel distance and low referral rates due to lack of awareness or skepticism. Facilitating factors included relying on resources such as professional networks and prioritizing outreach and education. Participants reported high professional satisfaction and were motivated to work in rural areas by personal experiences and qualities of the job such as being a generalist and having greater professional autonomy. These data demonstrate the feasibility of practicing in rural settings and suggest that in-person rural genetic counseling clinics may complement other strategies such as alternative service delivery models in increasing access for rural residents.

Published

2016