Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights

Sequencing of tumors is now routine and guides personalized cancer therapy. Mutant allele fractions (MAFs, or the ‘mutation dose’) of a driver gene may reveal the genomic structure of tumors and influence response to targeted therapies. We performed a comprehensive analysis of MAFs of driver alterat...

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Autores principales: Dienstmann, Rodrigo, Elez, Elena, Argiles, Guillem, Matos, Ignacio, Sanz‐Garcia, Enrique, Ortiz, Carolina, Macarulla, Teresa, Capdevila, Jaume, Alsina, Maria, Sauri, Tamara, Verdaguer, Helena, Vilaro, Marta, Ruiz‐Pace, Fiorella, Viaplana, Cristina, Garcia, Ariadna, Landolfi, Stefania, Palmer, Hector G., Nuciforo, Paolo, Rodon, Jordi, Vivancos, Ana, Tabernero, Josep
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5579330/
https://www.ncbi.nlm.nih.gov/pubmed/28618197
http://dx.doi.org/10.1002/1878-0261.12099
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author Dienstmann, Rodrigo
Elez, Elena
Argiles, Guillem
Matos, Ignacio
Sanz‐Garcia, Enrique
Ortiz, Carolina
Macarulla, Teresa
Capdevila, Jaume
Alsina, Maria
Sauri, Tamara
Verdaguer, Helena
Vilaro, Marta
Ruiz‐Pace, Fiorella
Viaplana, Cristina
Garcia, Ariadna
Landolfi, Stefania
Palmer, Hector G.
Nuciforo, Paolo
Rodon, Jordi
Vivancos, Ana
Tabernero, Josep
author_facet Dienstmann, Rodrigo
Elez, Elena
Argiles, Guillem
Matos, Ignacio
Sanz‐Garcia, Enrique
Ortiz, Carolina
Macarulla, Teresa
Capdevila, Jaume
Alsina, Maria
Sauri, Tamara
Verdaguer, Helena
Vilaro, Marta
Ruiz‐Pace, Fiorella
Viaplana, Cristina
Garcia, Ariadna
Landolfi, Stefania
Palmer, Hector G.
Nuciforo, Paolo
Rodon, Jordi
Vivancos, Ana
Tabernero, Josep
author_sort Dienstmann, Rodrigo
collection PubMed
description Sequencing of tumors is now routine and guides personalized cancer therapy. Mutant allele fractions (MAFs, or the ‘mutation dose’) of a driver gene may reveal the genomic structure of tumors and influence response to targeted therapies. We performed a comprehensive analysis of MAFs of driver alterations in unpaired primary and metastatic colorectal cancer (CRC) at our institution from 2010 to 2015 and studied their potential clinical relevance. Of 763 CRC samples, 622 had detailed annotation on overall survival in the metastatic setting (OSmet) and 89 received targeted agents matched to KRAS (MEK inhibitors), BRAF (BRAF inhibitors), or PIK3CA mutations (PI3K pathway inhibitors). MAFs of each variant were normalized for tumor purity in the sample (adjMAFs). We found lower adjMAFs for BRAF(V) (600E) and PIK3CA than for KRAS,NRAS, and BRAF non‐V600 variants. TP53 and BRAF(V) (600E) adjMAFs were higher in metastases as compared to primary tumors, and high KRAS adjMAFs were found in CRC metastases of patients with KRAS wild‐type primary tumors previously exposed to EGFR antibodies. Patients with RAS‐ or BRAF(V) (600E)‐mutated tumors, irrespective of adjMAFs, had worse OSmet. There was no significant association between adjMAFs and time to progression on targeted therapies matched to KRAS,BRAF, or PIK3CA mutations, potentially related to the limited antitumor activity of the employed drugs (overall response rate of 4.5%). In conclusion, the lower BRAF(V) (600E) and PIK3CA adjMAFs in subsets of primary CRC tumors indicate subclonality of these driver genes. Differences in adjMAFs between metastases and primary tumors suggest that approved therapies may result in selection of BRAF(V) (600E)‐ and KRAS‐resistant clones and an increase in genomic heterogeneity with acquired TP53 alterations. Despite significant differences in prognosis according to mutations in driver oncogenes, adjMAFs levels did not impact on survival and did not help predict benefit with matched targeted agents in the metastatic setting.
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spelling pubmed-55793302017-09-06 Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights Dienstmann, Rodrigo Elez, Elena Argiles, Guillem Matos, Ignacio Sanz‐Garcia, Enrique Ortiz, Carolina Macarulla, Teresa Capdevila, Jaume Alsina, Maria Sauri, Tamara Verdaguer, Helena Vilaro, Marta Ruiz‐Pace, Fiorella Viaplana, Cristina Garcia, Ariadna Landolfi, Stefania Palmer, Hector G. Nuciforo, Paolo Rodon, Jordi Vivancos, Ana Tabernero, Josep Mol Oncol Research Articles Sequencing of tumors is now routine and guides personalized cancer therapy. Mutant allele fractions (MAFs, or the ‘mutation dose’) of a driver gene may reveal the genomic structure of tumors and influence response to targeted therapies. We performed a comprehensive analysis of MAFs of driver alterations in unpaired primary and metastatic colorectal cancer (CRC) at our institution from 2010 to 2015 and studied their potential clinical relevance. Of 763 CRC samples, 622 had detailed annotation on overall survival in the metastatic setting (OSmet) and 89 received targeted agents matched to KRAS (MEK inhibitors), BRAF (BRAF inhibitors), or PIK3CA mutations (PI3K pathway inhibitors). MAFs of each variant were normalized for tumor purity in the sample (adjMAFs). We found lower adjMAFs for BRAF(V) (600E) and PIK3CA than for KRAS,NRAS, and BRAF non‐V600 variants. TP53 and BRAF(V) (600E) adjMAFs were higher in metastases as compared to primary tumors, and high KRAS adjMAFs were found in CRC metastases of patients with KRAS wild‐type primary tumors previously exposed to EGFR antibodies. Patients with RAS‐ or BRAF(V) (600E)‐mutated tumors, irrespective of adjMAFs, had worse OSmet. There was no significant association between adjMAFs and time to progression on targeted therapies matched to KRAS,BRAF, or PIK3CA mutations, potentially related to the limited antitumor activity of the employed drugs (overall response rate of 4.5%). In conclusion, the lower BRAF(V) (600E) and PIK3CA adjMAFs in subsets of primary CRC tumors indicate subclonality of these driver genes. Differences in adjMAFs between metastases and primary tumors suggest that approved therapies may result in selection of BRAF(V) (600E)‐ and KRAS‐resistant clones and an increase in genomic heterogeneity with acquired TP53 alterations. Despite significant differences in prognosis according to mutations in driver oncogenes, adjMAFs levels did not impact on survival and did not help predict benefit with matched targeted agents in the metastatic setting. John Wiley and Sons Inc. 2017-07-20 2017-09 /pmc/articles/PMC5579330/ /pubmed/28618197 http://dx.doi.org/10.1002/1878-0261.12099 Text en © 2017 The Authors. Published by FEBS Press and John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution (http://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
Dienstmann, Rodrigo
Elez, Elena
Argiles, Guillem
Matos, Ignacio
Sanz‐Garcia, Enrique
Ortiz, Carolina
Macarulla, Teresa
Capdevila, Jaume
Alsina, Maria
Sauri, Tamara
Verdaguer, Helena
Vilaro, Marta
Ruiz‐Pace, Fiorella
Viaplana, Cristina
Garcia, Ariadna
Landolfi, Stefania
Palmer, Hector G.
Nuciforo, Paolo
Rodon, Jordi
Vivancos, Ana
Tabernero, Josep
Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights
title Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights
title_full Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights
title_fullStr Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights
title_full_unstemmed Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights
title_short Analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights
title_sort analysis of mutant allele fractions in driver genes in colorectal cancer – biological and clinical insights
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5579330/
https://www.ncbi.nlm.nih.gov/pubmed/28618197
http://dx.doi.org/10.1002/1878-0261.12099
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