Your search keyword '"Scott W. Young"' showing total 2 results

1. Clinical Implementation of Integrated Genomic Profiling in Patients with Advanced Cancers

Author

Mitesh J. Borad, Jan B. Egan, Rachel M. Condjella, Winnie S. Liang, Rafael Fonseca, Nicole R. Ritacca, Ann E. McCullough, Michael T. Barrett, Katherine S. Hunt, Mia D. Champion, Maitray D. Patel, Scott W. Young, Alvin C. Silva, Thai H. Ho, Thorvardur R. Halfdanarson, Robert R. McWilliams, Konstantinos N. Lazaridis, Ramesh K. Ramanathan, Angela Baker, Jessica Aldrich, Ahmet Kurdoglu, Tyler Izatt, Alexis Christoforides, Irene Cherni, Sara Nasser, Rebecca Reiman, Lori Cuyugan, Jacquelyn McDonald, Jonathan Adkins, Stephen D. Mastrian, Riccardo Valdez, Dawn E. Jaroszewski, Daniel D. Von Hoff, David W. Craig, A. Keith Stewart, John D. Carpten, and Alan H. Bryce

Subjects

Medicine, Science

Abstract

Abstract DNA focused panel sequencing has been rapidly adopted to assess therapeutic targets in advanced/refractory cancer. Integrated Genomic Profiling (IGP) utilising DNA/RNA with tumour/normal comparisons in a Clinical Laboratory Improvement Amendments (CLIA) compliant setting enables a single assay to provide: therapeutic target prioritisation, novel target discovery/application and comprehensive germline assessment. A prospective study in 35 advanced/refractory cancer patients was conducted using CLIA-compliant IGP. Feasibility was assessed by estimating time to results (TTR), prioritising/assigning putative therapeutic targets, assessing drug access, ascertaining germline alterations, and assessing patient preferences/perspectives on data use/reporting. Therapeutic targets were identified using biointelligence/pathway analyses and interpreted by a Genomic Tumour Board. Seventy-five percent of cases harboured 1–3 therapeutically targetable mutations/case (median 79 mutations of potential functional significance/case). Median time to CLIA-validated results was 116 days with CLIA-validation of targets achieved in 21/22 patients. IGP directed treatment was instituted in 13 patients utilising on/off label FDA approved drugs (n = 9), clinical trials (n = 3) and single patient IND (n = 1). Preliminary clinical efficacy was noted in five patients (two partial response, three stable disease). Although barriers to broader application exist, including the need for wider availability of therapies, IGP in a CLIA-framework is feasible and valuable in selection/prioritisation of anti-cancer therapeutic targets.

Published

2016

2. Clinical Implementation of Integrated Genomic Profiling in Patients with Advanced Cancers

Author

Alvin C. Silva, Alexis Christoforides, Angela Baker, Michael T. Barrett, Rachel M. Condjella, Katherine S. Hunt, Dawn E. Jaroszewski, Tyler Izatt, Jacquelyn McDonald, Thai H. Ho, Mia D. Champion, Stephen D. Mastrian, Daniel D. Von Hoff, Riccardo Valdez, Ramesh K. Ramanathan, Winnie S. Liang, Thorvardur R. Halfdanarson, John D. Carpten, Konstantinos N. Lazaridis, A. Keith Stewart, Mitesh J. Borad, Maitray D. Patel, Irene Cherni, Ahmet Kurdoglu, Rebecca Reiman, Lori Cuyugan, Jessica Aldrich, David Craig, Alan H. Bryce, Ann E. McCullough, Robert R. McWilliams, Sara Nasser, Rafael Fonseca, Scott W. Young, Nicole R. Ritacca, Jonathan Adkins, and Jan B. Egan

Subjects

0301 basic medicine, Genomic profiling, Science, Drug Resistance, Genomics, Drug resistance, Bioinformatics, Off-label use, Article, 03 medical and health sciences, Neoplasms, Medicine, Humans, In patient, Clinical efficacy, Prospective Studies, Prospective cohort study, Multidisciplinary, business.industry, Diagnostic Tests, Routine, 3. Good health, Clinical trial, 030104 developmental biology, business

Abstract

DNA focused panel sequencing has been rapidly adopted to assess therapeutic targets in advanced/refractory cancer. Integrated Genomic Profiling (IGP) utilising DNA/RNA with tumour/normal comparisons in a Clinical Laboratory Improvement Amendments (CLIA) compliant setting enables a single assay to provide: therapeutic target prioritisation, novel target discovery/application and comprehensive germline assessment. A prospective study in 35 advanced/refractory cancer patients was conducted using CLIA-compliant IGP. Feasibility was assessed by estimating time to results (TTR), prioritising/assigning putative therapeutic targets, assessing drug access, ascertaining germline alterations, and assessing patient preferences/perspectives on data use/reporting. Therapeutic targets were identified using biointelligence/pathway analyses and interpreted by a Genomic Tumour Board. Seventy-five percent of cases harboured 1–3 therapeutically targetable mutations/case (median 79 mutations of potential functional significance/case). Median time to CLIA-validated results was 116 days with CLIA-validation of targets achieved in 21/22 patients. IGP directed treatment was instituted in 13 patients utilising on/off label FDA approved drugs (n = 9), clinical trials (n = 3) and single patient IND (n = 1). Preliminary clinical efficacy was noted in five patients (two partial response, three stable disease). Although barriers to broader application exist, including the need for wider availability of therapies, IGP in a CLIA-framework is feasible and valuable in selection/prioritisation of anti-cancer therapeutic targets.

Published

2016