Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay

PURPOSE: Gene fusions are established oncogenic drivers and emerging therapeutic targets in advanced colorectal cancer. This study aimed to detail the frequencies and clinicopathological features of gene fusions in colorectal cancer using a circulating tumor DNA assay. METHODS: Circulating tumor DNA...

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Autores principales: Clifton, Katherine, Rich, Thereasa A., Parseghian, Christine, Raymond, Victoria M., Dasari, Arvind, Pereira, Allan Andresson Lima, Willis, Jason, Loree, Jonathan M., Bauer, Todd M., Chae, Young Kwang, Sherrill, Gary, Fanta, Paul, Grothey, Axel, Hendifar, Andrew, Henry, David, Mahadevan, Daruka, Nezami, Mohammad Amin, Tan, Benjamin, Wainberg, Zev A., Lanman, Richard, Kopetz, Scott, Morris, Van
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Clinical Oncology 2019
Materias:
Original Reports
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7526699/
https://www.ncbi.nlm.nih.gov/pubmed/33015522
http://dx.doi.org/10.1200/PO.19.00141
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author Clifton, Katherine
Rich, Thereasa A.
Parseghian, Christine
Raymond, Victoria M.
Dasari, Arvind
Pereira, Allan Andresson Lima
Willis, Jason
Loree, Jonathan M.
Bauer, Todd M.
Chae, Young Kwang
Sherrill, Gary
Fanta, Paul
Grothey, Axel
Hendifar, Andrew
Henry, David
Mahadevan, Daruka
Nezami, Mohammad Amin
Tan, Benjamin
Wainberg, Zev A.
Lanman, Richard
Kopetz, Scott
Morris, Van
author_facet Clifton, Katherine
Rich, Thereasa A.
Parseghian, Christine
Raymond, Victoria M.
Dasari, Arvind
Pereira, Allan Andresson Lima
Willis, Jason
Loree, Jonathan M.
Bauer, Todd M.
Chae, Young Kwang
Sherrill, Gary
Fanta, Paul
Grothey, Axel
Hendifar, Andrew
Henry, David
Mahadevan, Daruka
Nezami, Mohammad Amin
Tan, Benjamin
Wainberg, Zev A.
Lanman, Richard
Kopetz, Scott
Morris, Van
author_sort Clifton, Katherine
collection PubMed
description PURPOSE: Gene fusions are established oncogenic drivers and emerging therapeutic targets in advanced colorectal cancer. This study aimed to detail the frequencies and clinicopathological features of gene fusions in colorectal cancer using a circulating tumor DNA assay. METHODS: Circulating tumor DNA samples in patients with advanced colorectal cancer were analyzed at 4,581 unique time points using a validated plasma-based multigene assay that includes assessment of fusions in FGFR2, FGFR3, RET, ALK, NTRK1, and ROS1. Associations between fusions and clinicopathological features were measured using Fisher’s exact test. Relative frequencies of genomic alterations were compared between fusion-present and fusion-absent cases using an unpaired t test. RESULTS: Forty-four unique fusions were identified in 40 (1.1%) of the 3,808 patients with circulating tumor DNA detected: RET (n = 6; 36% of all fusions detected), FGFR3 (n = 2; 27%), ALK (n = 10, 23%), NTRK1 (n = 3; 7%), ROS1 (n = 2; 5%), and FGFR2 (n = 1; 2%). Relative to nonfusion variants detected, fusions were more likely to be subclonal (odds ratio, 8.2; 95% CI, 2.94 to 23.00; P < .001). Mutations associated with a previously reported anti–epidermal growth factor receptor (anti-EGFR) therapy resistance signature (subclonal RAS and EGFR mutations) were found with fusions in FGFR3 (10 of 12 patients), RET (nine of 16 patients), and ALK (seven of 10 patients). For the 27 patients with available clinical histories, 21 (78%) had EGFR monoclonal antibody treatment before fusion detection. CONCLUSION: Diverse and potentially actionable fusions can be detected using a circulating tumor DNA assay in patients with advanced colorectal cancer. Distribution of coexisting subclonal mutations in EGFR, KRAS, and NRAS in a subset of the patients with fusion-present colorectal cancer suggests that these fusions may arise as a novel mechanism of resistance to anti-EGFR therapies in patients with metastatic colorectal cancer.
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spelling pubmed-75266992020-10-02 Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay Clifton, Katherine Rich, Thereasa A. Parseghian, Christine Raymond, Victoria M. Dasari, Arvind Pereira, Allan Andresson Lima Willis, Jason Loree, Jonathan M. Bauer, Todd M. Chae, Young Kwang Sherrill, Gary Fanta, Paul Grothey, Axel Hendifar, Andrew Henry, David Mahadevan, Daruka Nezami, Mohammad Amin Tan, Benjamin Wainberg, Zev A. Lanman, Richard Kopetz, Scott Morris, Van JCO Precis Oncol Original Reports PURPOSE: Gene fusions are established oncogenic drivers and emerging therapeutic targets in advanced colorectal cancer. This study aimed to detail the frequencies and clinicopathological features of gene fusions in colorectal cancer using a circulating tumor DNA assay. METHODS: Circulating tumor DNA samples in patients with advanced colorectal cancer were analyzed at 4,581 unique time points using a validated plasma-based multigene assay that includes assessment of fusions in FGFR2, FGFR3, RET, ALK, NTRK1, and ROS1. Associations between fusions and clinicopathological features were measured using Fisher’s exact test. Relative frequencies of genomic alterations were compared between fusion-present and fusion-absent cases using an unpaired t test. RESULTS: Forty-four unique fusions were identified in 40 (1.1%) of the 3,808 patients with circulating tumor DNA detected: RET (n = 6; 36% of all fusions detected), FGFR3 (n = 2; 27%), ALK (n = 10, 23%), NTRK1 (n = 3; 7%), ROS1 (n = 2; 5%), and FGFR2 (n = 1; 2%). Relative to nonfusion variants detected, fusions were more likely to be subclonal (odds ratio, 8.2; 95% CI, 2.94 to 23.00; P < .001). Mutations associated with a previously reported anti–epidermal growth factor receptor (anti-EGFR) therapy resistance signature (subclonal RAS and EGFR mutations) were found with fusions in FGFR3 (10 of 12 patients), RET (nine of 16 patients), and ALK (seven of 10 patients). For the 27 patients with available clinical histories, 21 (78%) had EGFR monoclonal antibody treatment before fusion detection. CONCLUSION: Diverse and potentially actionable fusions can be detected using a circulating tumor DNA assay in patients with advanced colorectal cancer. Distribution of coexisting subclonal mutations in EGFR, KRAS, and NRAS in a subset of the patients with fusion-present colorectal cancer suggests that these fusions may arise as a novel mechanism of resistance to anti-EGFR therapies in patients with metastatic colorectal cancer. American Society of Clinical Oncology 2019-10-03 /pmc/articles/PMC7526699/ /pubmed/33015522 http://dx.doi.org/10.1200/PO.19.00141 Text en © 2019 by American Society of Clinical Oncology https://creativecommons.org/licenses/by/4.0/ Licensed under the Creative Commons Attribution 4.0 License: https://creativecommons.org/licenses/by/4.0/
spellingShingle Original Reports
Clifton, Katherine
Rich, Thereasa A.
Parseghian, Christine
Raymond, Victoria M.
Dasari, Arvind
Pereira, Allan Andresson Lima
Willis, Jason
Loree, Jonathan M.
Bauer, Todd M.
Chae, Young Kwang
Sherrill, Gary
Fanta, Paul
Grothey, Axel
Hendifar, Andrew
Henry, David
Mahadevan, Daruka
Nezami, Mohammad Amin
Tan, Benjamin
Wainberg, Zev A.
Lanman, Richard
Kopetz, Scott
Morris, Van
Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay
title Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay
title_full Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay
title_fullStr Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay
title_full_unstemmed Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay
title_short Identification of Actionable Fusions as an Anti-EGFR Resistance Mechanism Using a Circulating Tumor DNA Assay
title_sort identification of actionable fusions as an anti-egfr resistance mechanism using a circulating tumor dna assay
topic Original Reports
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7526699/
https://www.ncbi.nlm.nih.gov/pubmed/33015522
http://dx.doi.org/10.1200/PO.19.00141
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