Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection

Nearly all estrogen receptor (ER)‐positive (POS) metastatic breast cancers become refractory to endocrine (ET) and other therapies, leading to lethal disease presumably due to evolving genomic alterations. Timely monitoring of the molecular events associated with response/progression by serial tissu...

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Autores principales: Cani, Andi K., Dolce, Emily M., Darga, Elizabeth P., Hu, Kevin, Liu, Chia‐Jen, Pierce, Jackie, Bradbury, Kieran, Kilgour, Elaine, Aung, Kimberly, Schiavon, Gaia, Carroll, Danielle, Carr, T. Hedley, Klinowska, Teresa, Lindemann, Justin, Marshall, Gayle, Rowlands, Vicky, Harrington, Elizabeth A., Barrett, J. Carl, Sathiyayogan, Nitharsan, Morrow, Christopher, Sero, Valeria, Armstrong, Anne C., Baird, Richard, Hamilton, Erika, Im, Seock‐Ah, Jhaveri, Komal, Patel, Manish R., Dive, Caroline, Tomlins, Scott A., Udager, Aaron M., Hayes, Daniel F., Paoletti, Costanza
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9120891/
https://www.ncbi.nlm.nih.gov/pubmed/34866317
http://dx.doi.org/10.1002/1878-0261.13150
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author Cani, Andi K.
Dolce, Emily M.
Darga, Elizabeth P.
Hu, Kevin
Liu, Chia‐Jen
Pierce, Jackie
Bradbury, Kieran
Kilgour, Elaine
Aung, Kimberly
Schiavon, Gaia
Carroll, Danielle
Carr, T. Hedley
Klinowska, Teresa
Lindemann, Justin
Marshall, Gayle
Rowlands, Vicky
Harrington, Elizabeth A.
Barrett, J. Carl
Sathiyayogan, Nitharsan
Morrow, Christopher
Sero, Valeria
Armstrong, Anne C.
Baird, Richard
Hamilton, Erika
Im, Seock‐Ah
Jhaveri, Komal
Patel, Manish R.
Dive, Caroline
Tomlins, Scott A.
Udager, Aaron M.
Hayes, Daniel F.
Paoletti, Costanza
author_facet Cani, Andi K.
Dolce, Emily M.
Darga, Elizabeth P.
Hu, Kevin
Liu, Chia‐Jen
Pierce, Jackie
Bradbury, Kieran
Kilgour, Elaine
Aung, Kimberly
Schiavon, Gaia
Carroll, Danielle
Carr, T. Hedley
Klinowska, Teresa
Lindemann, Justin
Marshall, Gayle
Rowlands, Vicky
Harrington, Elizabeth A.
Barrett, J. Carl
Sathiyayogan, Nitharsan
Morrow, Christopher
Sero, Valeria
Armstrong, Anne C.
Baird, Richard
Hamilton, Erika
Im, Seock‐Ah
Jhaveri, Komal
Patel, Manish R.
Dive, Caroline
Tomlins, Scott A.
Udager, Aaron M.
Hayes, Daniel F.
Paoletti, Costanza
author_sort Cani, Andi K.
collection PubMed
description Nearly all estrogen receptor (ER)‐positive (POS) metastatic breast cancers become refractory to endocrine (ET) and other therapies, leading to lethal disease presumably due to evolving genomic alterations. Timely monitoring of the molecular events associated with response/progression by serial tissue biopsies is logistically difficult. Use of liquid biopsies, including circulating tumor cells (CTC) and circulating tumor DNA (ctDNA), might provide highly informative, yet easily obtainable, evidence for better precision oncology care. Although ctDNA profiling has been well investigated, the CTC precision oncology genomic landscape and the advantages it may offer over ctDNA in ER‐POS breast cancer remain largely unexplored. Whole‐blood (WB) specimens were collected at serial time points from patients with advanced ER‐POS/HER2‐negative (NEG) advanced breast cancer in a phase I trial of AZD9496, an oral selective ER degrader (SERD) ET. Individual CTC were isolated from WB using tandem CellSearch(®)/DEPArray™ technologies and genomically profiled by targeted single‐cell DNA next‐generation sequencing (scNGS). High‐quality CTC (n = 123) from 12 patients profiled by scNGS showed 100% concordance with ctDNA detection of driver estrogen receptor α (ESR1) mutations. We developed a novel CTC‐based framework for precision medicine actionability reporting (MI‐CTCseq) that incorporates novel features, such as clonal predominance and zygosity of targetable alterations, both unambiguously identifiable in CTC compared to ctDNA. Thus, we nominated opportunities for targeted therapies in 73% of patients, directed at alterations in phosphatidylinositol‐4,5‐bisphosphate 3‐kinase catalytic subunit alpha (PIK3CA), fibroblast growth factor receptor 2 (FGFR2), and KIT proto‐oncogene, receptor tyrosine kinase (KIT). Intrapatient, inter‐CTC genomic heterogeneity was observed, at times between time points, in subclonal alterations. Our analysis suggests that serial monitoring of the CTC genome is feasible and should enable real‐time tracking of tumor evolution during progression, permitting more combination precision medicine interventions.
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spelling pubmed-91208912022-05-21 Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection Cani, Andi K. Dolce, Emily M. Darga, Elizabeth P. Hu, Kevin Liu, Chia‐Jen Pierce, Jackie Bradbury, Kieran Kilgour, Elaine Aung, Kimberly Schiavon, Gaia Carroll, Danielle Carr, T. Hedley Klinowska, Teresa Lindemann, Justin Marshall, Gayle Rowlands, Vicky Harrington, Elizabeth A. Barrett, J. Carl Sathiyayogan, Nitharsan Morrow, Christopher Sero, Valeria Armstrong, Anne C. Baird, Richard Hamilton, Erika Im, Seock‐Ah Jhaveri, Komal Patel, Manish R. Dive, Caroline Tomlins, Scott A. Udager, Aaron M. Hayes, Daniel F. Paoletti, Costanza Mol Oncol Research Articles Nearly all estrogen receptor (ER)‐positive (POS) metastatic breast cancers become refractory to endocrine (ET) and other therapies, leading to lethal disease presumably due to evolving genomic alterations. Timely monitoring of the molecular events associated with response/progression by serial tissue biopsies is logistically difficult. Use of liquid biopsies, including circulating tumor cells (CTC) and circulating tumor DNA (ctDNA), might provide highly informative, yet easily obtainable, evidence for better precision oncology care. Although ctDNA profiling has been well investigated, the CTC precision oncology genomic landscape and the advantages it may offer over ctDNA in ER‐POS breast cancer remain largely unexplored. Whole‐blood (WB) specimens were collected at serial time points from patients with advanced ER‐POS/HER2‐negative (NEG) advanced breast cancer in a phase I trial of AZD9496, an oral selective ER degrader (SERD) ET. Individual CTC were isolated from WB using tandem CellSearch(®)/DEPArray™ technologies and genomically profiled by targeted single‐cell DNA next‐generation sequencing (scNGS). High‐quality CTC (n = 123) from 12 patients profiled by scNGS showed 100% concordance with ctDNA detection of driver estrogen receptor α (ESR1) mutations. We developed a novel CTC‐based framework for precision medicine actionability reporting (MI‐CTCseq) that incorporates novel features, such as clonal predominance and zygosity of targetable alterations, both unambiguously identifiable in CTC compared to ctDNA. Thus, we nominated opportunities for targeted therapies in 73% of patients, directed at alterations in phosphatidylinositol‐4,5‐bisphosphate 3‐kinase catalytic subunit alpha (PIK3CA), fibroblast growth factor receptor 2 (FGFR2), and KIT proto‐oncogene, receptor tyrosine kinase (KIT). Intrapatient, inter‐CTC genomic heterogeneity was observed, at times between time points, in subclonal alterations. Our analysis suggests that serial monitoring of the CTC genome is feasible and should enable real‐time tracking of tumor evolution during progression, permitting more combination precision medicine interventions. John Wiley and Sons Inc. 2021-12-20 2022-05 /pmc/articles/PMC9120891/ /pubmed/34866317 http://dx.doi.org/10.1002/1878-0261.13150 Text en © 2021 The Authors. Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Cani, Andi K.
Dolce, Emily M.
Darga, Elizabeth P.
Hu, Kevin
Liu, Chia‐Jen
Pierce, Jackie
Bradbury, Kieran
Kilgour, Elaine
Aung, Kimberly
Schiavon, Gaia
Carroll, Danielle
Carr, T. Hedley
Klinowska, Teresa
Lindemann, Justin
Marshall, Gayle
Rowlands, Vicky
Harrington, Elizabeth A.
Barrett, J. Carl
Sathiyayogan, Nitharsan
Morrow, Christopher
Sero, Valeria
Armstrong, Anne C.
Baird, Richard
Hamilton, Erika
Im, Seock‐Ah
Jhaveri, Komal
Patel, Manish R.
Dive, Caroline
Tomlins, Scott A.
Udager, Aaron M.
Hayes, Daniel F.
Paoletti, Costanza
Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection
title Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection
title_full Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection
title_fullStr Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection
title_full_unstemmed Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection
title_short Serial monitoring of genomic alterations in circulating tumor cells of ER‐positive/HER2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection
title_sort serial monitoring of genomic alterations in circulating tumor cells of er‐positive/her2‐negative advanced breast cancer: feasibility of precision oncology biomarker detection
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9120891/
https://www.ncbi.nlm.nih.gov/pubmed/34866317
http://dx.doi.org/10.1002/1878-0261.13150
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