Your search keyword '"Miren Sagardia, A"' showing total 8 results

1. Secondary findings from clinical genomic sequencing: prevalence, patient perspectives, family history assessment, and health-care costs from a multisite study

Author

Hart, M. Ragan, Biesecker, Barbara B., Blout, Carrie L., Christensen, Kurt D., Amendola, Laura M., Bergstrom, Katie L., Biswas, Sawona, Bowling, Kevin M., Brothers, Kyle B., Conlin, Laura K., Cooper, Greg M., Dulik, Matthew C., East, Kelly M., Everett, Jessica N., Finnila, Candice R., Ghazani, Arezou A., Gilmore, Marian J., Goddard, Katrina A. B, Jarvik, Gail P., Johnston, Jennifer J., Kauffman, Tia L., Kelley, Whitley V., Krier, Joel B., Lewis, Katie L., McGuire, Amy L., McMullen, Carmit, Ou, Jeffrey, Plon, Sharon E., Rehm, Heidi L., Richards, C. Sue, Romasko, Edward J., Miren Sagardia, Ane, Spinner, Nancy B., Thompson, Michelle L., Turbitt, Erin, Vassy, Jason L., Wilfond, Benjamin S., Veenstra, David L., Berg, Jonathan S., Green, Robert C., Biesecker, Leslie G., and Hindorff, Lucia A.

Published

2019

2. Evaluation of Recipients of Positive and Negative Secondary Findings Evaluations in a Hybrid CLIA-Research Sequencing Pilot

Author

Barnabas, Beatrice B., Bouffard, Gerard G., Brooks, Shelise Y., Coleman, Holly, Dekhtyar, Lyudmila, Guan, Xiaobin, Han, Joel, Ho, Shi-ling, Legaspi, Richelle, Maduro, Quino L., Masiello, Catherine A., McDowell, Jennifer C., Montemayor, Casandra, Park, Morgan, Riebow, Nancy L., Schandler, Karen, Scharer, Chanthra, Schmidt, Brian, Sison, Christina, Stantripop, Sirintorn, Thomas, James W., Thomas, Pamela J., Vemulapalli, Meghana, Young, Alice C., Sapp, Julie C., Johnston, Jennifer J., Driscoll, Kate, Heidlebaugh, Alexis R., Miren Sagardia, Ane, Dogbe, D. Nadine, Umstead, Kendall L., Turbitt, Erin, Alevizos, Ilias, Baron, Jeffrey, Bönnemann, Carsten, Brooks, Brian, Donkervoort, Sandra, Jee, Youn Hee, Linehan, W. Marston, McMahon, Francis J., Moss, Joel, Mullikin, James C., Nielsen, Deborah, Pelayo, Eileen, Remaley, Alan T., Siegel, Richard, Su, Helen, Zarate, Carlos, Manolio, Teri A., Biesecker, Barbara B., and Biesecker, Leslie G.

Published

2018

3. Evaluation of Recipients of Positive and Negative Secondary Findings Evaluations in a Hybrid CLIA-Research Sequencing Pilot

Author

Carsten G. Bönnemann, Francis J. McMahon, Quino Maduro, Alan T. Remaley, Brian P. Brooks, Sirintorn Stantripop, Jennifer C. McDowell, Kendall L. Umstead, Gerard G. Bouffard, Erin Turbitt, Catherine A. Masiello, Karen Schandler, Jeffrey Baron, Jennifer J. Johnston, Beatrice B. Barnabas, Richelle Legaspi, James W. Thomas, Holly Coleman, Eileen Pelayo, Barbara B. Biesecker, D. Nadine Dogbe, Ilias Alevizos, Joel Moss, W. Marston Linehan, Helen C. Su, Casandra Montemayor, Brian Schmidt, Alice C. Young, Morgan Park, Meghana Vemulapalli, Richard M. Siegel, Pamela J. Thomas, Chanthra Scharer, Youn Hee Jee, Deborah Nielsen, Carlos A. Zarate, Christina Sison, Leslie G. Biesecker, Alexis R Heidlebaugh, Sandra Donkervoort, Nancy Riebow, Shelise Brooks, James C. Mullikin, Teri A. Manolio, Julie C. Sapp, Xiaobin Guan, Ane Miren Sagardia, S. L. Ho, Kate Driscoll, Joel Han, and Lyudmila Dekhtyar

Subjects

0301 basic medicine, Male, medicine.medical_specialty, media_common.quotation_subject, Genetic counseling, Specialty, Genetic Counseling, Pilot Projects, 030105 genetics & heredity, Article, 03 medical and health sciences, 0302 clinical medicine, Health care, Genetics, medicine, Humans, Exome, Genetics (clinical), Exome sequencing, media_common, Protocol (science), Receipt, Genetics & Heredity, Incidental Findings, business.industry, Psychologic distress, Genomics, Middle Aged, Surprise, 030220 oncology & carcinogenesis, Family medicine, Female, business

Abstract

© 2018 While consensus regarding the return of secondary genomic findings in the clinical setting has been reached, debate about such findings in the research setting remains. We developed a hybrid, research-clinical translational genomics process for research exome data coupled with a CLIA-validated secondary findings analysis. Eleven intramural investigators from ten institutes at the National Institutes of Health piloted this process. Nearly 1,200 individuals were sequenced and 14 secondary findings were identified in 18 participants. Positive secondary findings were returned by a genetic counselor following a standardized protocol, including referrals for specialty follow-up care for the secondary finding local to the participants. Interviews were undertaken with 13 participants 4 months after receipt of a positive report. These participants reported minimal psychologic distress within a process to assimilate their results. Of the 13, 9 reported accessing the recommended health care services. A sample of 107 participants who received a negative findings report were surveyed 4 months after receiving it. They demonstrated good understanding of the negative secondary findings result and most expressed reassurance (64%) from that report. However, a notable minority (up to 17%) expressed confusion regarding the distinction of primary from secondary findings. This pilot shows it is feasible to couple CLIA-compliant secondary findings to research sequencing with minimal harms. Participants managed the surprise of a secondary finding with most following recommended follow up, yet some with negative findings conflated secondary and primary findings. Additional work is needed to understand barriers to follow-up care and help participants distinguish secondary from primary findings.

Published

2018

4. Secondary findings from clinical genomic sequencing: prevalence, patient perspectives, family history assessment, and health-care costs from a multisite study

Author

Tia L. Kauffman, Carmit K. McMullen, Greg M. Cooper, Marian J. Gilmore, Edward J. Romasko, Carrie L. Blout, Jennifer J. Johnston, Ragan Hart, Amy L. McGuire, Robert C. Green, Kevin M. Bowling, Leslie G. Biesecker, Joel B. Krier, Nancy B. Spinner, Heidi L. Rehm, Candice R. Finnila, Benjamin S. Wilfond, Arezou A. Ghazani, Jonathan S. Berg, Laura K. Conlin, Ane Miren Sagardia, Katie L. Lewis, Matthew C. Dulik, Gail P. Jarvik, Lucia A. Hindorff, Michelle L. Thompson, Sharon E. Plon, Erin Turbitt, Kurt D. Christensen, Jason L. Vassy, Kelly M. East, Whitley V. Kelley, David L. Veenstra, C. Sue Richards, Katrina A.B. Goddard, Jeffrey Ou, Barbara B. Biesecker, Jessica Everett, Katie Bergstrom, Laura M. Amendola, and Sawona Biswas

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Health Knowledge, Attitudes, Practice, Patients, Health Personnel, Decision Making, MEDLINE, Disclosure, Intention, 030105 genetics & heredity, Article, 03 medical and health sciences, Health care, medicine, Prevalence, Humans, Exome, Genetic Testing, Family history, Genetics (clinical), Genetics & Heredity, Incidental Findings, Whole Genome Sequencing, business.industry, Published Erratum, Genomic sequencing, High-Throughput Nucleotide Sequencing, Genomics, Health Care Costs, 030104 developmental biology, Family medicine, Female, business

Abstract

© 2018, American College of Medical Genetics and Genomics. Purpose: Clinical sequencing emerging in health care may result in secondary findings (SFs). Methods: Seventy-four of 6240 (1.2%) participants who underwent genome or exome sequencing through the Clinical Sequencing Exploratory Research (CSER) Consortium received one or more SFs from the original American College of Medical Genetics and Genomics (ACMG) recommended 56 gene–condition pair list; we assessed clinical and psychosocial actions. Results: The overall adjusted prevalence of SFs in the ACMG 56 genes across the CSER consortium was 1.7%. Initially 32% of the family histories were positive, and post disclosure, this increased to 48%. The average cost of follow-up medical actions per finding up to a 1-year period was $128 (observed, range: $0–$678) and $421 (recommended, range: $141–$1114). Case reports revealed variability in the frequency of and follow-up on medical recommendations patients received associated with each SF gene–condition pair. Participants did not report adverse psychosocial impact associated with receiving SFs; this was corroborated by 18 participant (or parent) interviews. All interviewed participants shared findings with relatives and reported that relatives did not pursue additional testing or care. Conclusion: Our results suggest that disclosure of SFs shows little to no adverse impact on participants and adds only modestly to near-term health-care costs; additional studies are needed to confirm these findings.

Published

2018

5. Correction: Secondary findings from clinical genomic sequencing: prevalence, patient perspectives, family history assessment, and health-care costs from a multisite study

Author

Nancy B. Spinner, Katie L. Lewis, Sawona Biswas, Marian J. Gilmore, Carrie L. Blout, Edward J. Romasko, Laura M. Amendola, Matthew C. Dulik, Jeffrey Ou, Leslie G. Biesecker, C. Sue Richards, Tia L. Kauffman, Carmit K. McMullen, Candice R. Finnila, Kevin M. Bowling, Jessica Everett, Robert C. Green, Lucia A. Hindorff, Barbara B. Biesecker, Sharon E. Plon, Katie Bergstrom, Amy L. McGuire, Benjamin S. Wilfond, Arezou A. Ghazani, David L. Veenstra, Jason L. Vassy, Laura K. Conlin, Michelle L. Thompson, Greg M. Cooper, Joel B. Krier, Kelly M. East, Gail P. Jarvik, Whitley V. Kelley, Jonathan S. Berg, Ane Miren Sagardia, Erin Turbitt, Kurt D. Christensen, Ragan Hart, Jennifer J. Johnston, Heidi L. Rehm, and Katrina A.B. Goddard

Subjects

medicine.medical_specialty, business.industry, Genomic sequencing, Family medicine, Health care, Medicine, Family history, business, Genetics (clinical)

Published

2019

6. Secondary findings from clinical genomic sequencing: prevalence, patient perspectives, family history assessment, and health-care costs from a multisite study

Author

Hart, MR, Biesecker, BB, Blout, CL, Christensen, KD, Amendola, LM, Bergstrom, KL, Biswas, S, Bowling, KM, Brothers, KB, Conlin, LK, Cooper, GM, Dulik, MC, East, KM, Everett, JN, Finnila, CR, Ghazani, AA, Gilmore, MJ, Goddard, KAB, Jarvik, GP, Johnston, JJ, Kauffman, TL, Kelley, WV, Krier, JB, Lewis, KL, McGuire, AL, McMullen, C, Ou, J, Plon, SE, Rehm, HL, Richards, CS, Romasko, EJ, Miren Sagardia, A, Spinner, NB, Thompson, ML, Turbitt, E, Vassy, JL, Wilfond, BS, Veenstra, DL, Berg, JS, Green, RC, Biesecker, LG, Hindorff, LA, Hart, MR, Biesecker, BB, Blout, CL, Christensen, KD, Amendola, LM, Bergstrom, KL, Biswas, S, Bowling, KM, Brothers, KB, Conlin, LK, Cooper, GM, Dulik, MC, East, KM, Everett, JN, Finnila, CR, Ghazani, AA, Gilmore, MJ, Goddard, KAB, Jarvik, GP, Johnston, JJ, Kauffman, TL, Kelley, WV, Krier, JB, Lewis, KL, McGuire, AL, McMullen, C, Ou, J, Plon, SE, Rehm, HL, Richards, CS, Romasko, EJ, Miren Sagardia, A, Spinner, NB, Thompson, ML, Turbitt, E, Vassy, JL, Wilfond, BS, Veenstra, DL, Berg, JS, Green, RC, Biesecker, LG, and Hindorff, LA

Abstract

© 2018, American College of Medical Genetics and Genomics. Purpose: Clinical sequencing emerging in health care may result in secondary findings (SFs). Methods: Seventy-four of 6240 (1.2%) participants who underwent genome or exome sequencing through the Clinical Sequencing Exploratory Research (CSER) Consortium received one or more SFs from the original American College of Medical Genetics and Genomics (ACMG) recommended 56 gene–condition pair list; we assessed clinical and psychosocial actions. Results: The overall adjusted prevalence of SFs in the ACMG 56 genes across the CSER consortium was 1.7%. Initially 32% of the family histories were positive, and post disclosure, this increased to 48%. The average cost of follow-up medical actions per finding up to a 1-year period was $128 (observed, range: $0–$678) and $421 (recommended, range: $141–$1114). Case reports revealed variability in the frequency of and follow-up on medical recommendations patients received associated with each SF gene–condition pair. Participants did not report adverse psychosocial impact associated with receiving SFs; this was corroborated by 18 participant (or parent) interviews. All interviewed participants shared findings with relatives and reported that relatives did not pursue additional testing or care. Conclusion: Our results suggest that disclosure of SFs shows little to no adverse impact on participants and adds only modestly to near-term health-care costs; additional studies are needed to confirm these findings.

Published

2019

7. Evaluation of Recipients of Positive and Negative Secondary Findings Evaluations in a Hybrid CLIA-Research Sequencing Pilot

Author

Sapp, Julie C., primary, Johnston, Jennifer J., additional, Driscoll, Kate, additional, Heidlebaugh, Alexis R., additional, Miren Sagardia, Ane, additional, Dogbe, D. Nadine, additional, Umstead, Kendall L., additional, Turbitt, Erin, additional, Alevizos, Ilias, additional, Baron, Jeffrey, additional, Bönnemann, Carsten, additional, Brooks, Brian, additional, Donkervoort, Sandra, additional, Jee, Youn Hee, additional, Linehan, W. Marston, additional, McMahon, Francis J., additional, Moss, Joel, additional, Mullikin, James C., additional, Nielsen, Deborah, additional, Pelayo, Eileen, additional, Remaley, Alan T., additional, Siegel, Richard, additional, Su, Helen, additional, Zarate, Carlos, additional, Manolio, Teri A., additional, Biesecker, Barbara B., additional, Biesecker, Leslie G., additional, Barnabas, Beatrice B., additional, Bouffard, Gerard G., additional, Brooks, Shelise Y., additional, Coleman, Holly, additional, Dekhtyar, Lyudmila, additional, Guan, Xiaobin, additional, Han, Joel, additional, Ho, Shi-ling, additional, Legaspi, Richelle, additional, Maduro, Quino L., additional, Masiello, Catherine A., additional, McDowell, Jennifer C., additional, Montemayor, Casandra, additional, Park, Morgan, additional, Riebow, Nancy L., additional, Schandler, Karen, additional, Scharer, Chanthra, additional, Schmidt, Brian, additional, Sison, Christina, additional, Stantripop, Sirintorn, additional, Thomas, James W., additional, Thomas, Pamela J., additional, Vemulapalli, Meghana, additional, and Young, Alice C., additional

Published

2018

8. Evaluation of Recipients of Positive and Negative Secondary Findings Evaluations in a Hybrid CLIA-Research Sequencing Pilot

Author

Sapp, JC, Johnston, JJ, Driscoll, K, Heidlebaugh, AR, Miren Sagardia, A, Dogbe, DN, Umstead, KL, Turbitt, E, Alevizos, I, Baron, J, Bönnemann, C, Brooks, B, Donkervoort, S, Jee, YH, Linehan, WM, McMahon, FJ, Moss, J, Mullikin, JC, Nielsen, D, Pelayo, E, Remaley, AT, Siegel, R, Su, H, Zarate, C, Barnabas, BB, Bouffard, GG, Brooks, SY, Coleman, H, Dekhtyar, L, Guan, X, Han, J, Ho, SL, Legaspi, R, Maduro, QL, Masiello, CA, McDowell, JC, Montemayor, C, Park, M, Riebow, NL, Schandler, K, Scharer, C, Schmidt, B, Sison, C, Stantripop, S, Thomas, JW, Thomas, PJ, Vemulapalli, M, Young, AC, Manolio, TA, Biesecker, BB, Biesecker, LG, Sapp, JC, Johnston, JJ, Driscoll, K, Heidlebaugh, AR, Miren Sagardia, A, Dogbe, DN, Umstead, KL, Turbitt, E, Alevizos, I, Baron, J, Bönnemann, C, Brooks, B, Donkervoort, S, Jee, YH, Linehan, WM, McMahon, FJ, Moss, J, Mullikin, JC, Nielsen, D, Pelayo, E, Remaley, AT, Siegel, R, Su, H, Zarate, C, Barnabas, BB, Bouffard, GG, Brooks, SY, Coleman, H, Dekhtyar, L, Guan, X, Han, J, Ho, SL, Legaspi, R, Maduro, QL, Masiello, CA, McDowell, JC, Montemayor, C, Park, M, Riebow, NL, Schandler, K, Scharer, C, Schmidt, B, Sison, C, Stantripop, S, Thomas, JW, Thomas, PJ, Vemulapalli, M, Young, AC, Manolio, TA, Biesecker, BB, and Biesecker, LG

Abstract

© 2018 While consensus regarding the return of secondary genomic findings in the clinical setting has been reached, debate about such findings in the research setting remains. We developed a hybrid, research-clinical translational genomics process for research exome data coupled with a CLIA-validated secondary findings analysis. Eleven intramural investigators from ten institutes at the National Institutes of Health piloted this process. Nearly 1,200 individuals were sequenced and 14 secondary findings were identified in 18 participants. Positive secondary findings were returned by a genetic counselor following a standardized protocol, including referrals for specialty follow-up care for the secondary finding local to the participants. Interviews were undertaken with 13 participants 4 months after receipt of a positive report. These participants reported minimal psychologic distress within a process to assimilate their results. Of the 13, 9 reported accessing the recommended health care services. A sample of 107 participants who received a negative findings report were surveyed 4 months after receiving it. They demonstrated good understanding of the negative secondary findings result and most expressed reassurance (64%) from that report. However, a notable minority (up to 17%) expressed confusion regarding the distinction of primary from secondary findings. This pilot shows it is feasible to couple CLIA-compliant secondary findings to research sequencing with minimal harms. Participants managed the surprise of a secondary finding with most following recommended follow up, yet some with negative findings conflated secondary and primary findings. Additional work is needed to understand barriers to follow-up care and help participants distinguish secondary from primary findings.

Published

2018