Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers

The RAS family of small GTPases represents the most commonly activated oncogenes in human cancers. To better understand the prevalence of somatic RAS mutations and the compendium of genes that are coaltered in RAS-mutant tumors, we analyzed targeted next-generation sequencing data of 607,863 mutatio...

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Autores principales: Scharpf, Robert B., Balan, Archana, Ricciuti, Biagio, Fiksel, Jacob, Cherry, Christopher, Wang, Chenguang, Lenoue-Newton, Michele L., Rizvi, Hira A., White, James R., Baras, Alexander S., Anaya, Jordan, Landon, Blair V., Majcherska-Agrawal, Marta, Ghanem, Paola, Lee, Jocelyn, Raskin, Leon, Park, Andrew S., Tu, Huakang, Hsu, Hil, Arbour, Kathryn C., Awad, Mark M., Riely, Gregory J., Lovly, Christine M., Anagnostou, Valsamo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2022
Materias:
Translational Science
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9627127/
https://www.ncbi.nlm.nih.gov/pubmed/36074020
http://dx.doi.org/10.1158/0008-5472.CAN-22-1731
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author Scharpf, Robert B.
Balan, Archana
Ricciuti, Biagio
Fiksel, Jacob
Cherry, Christopher
Wang, Chenguang
Lenoue-Newton, Michele L.
Rizvi, Hira A.
White, James R.
Baras, Alexander S.
Anaya, Jordan
Landon, Blair V.
Majcherska-Agrawal, Marta
Ghanem, Paola
Lee, Jocelyn
Raskin, Leon
Park, Andrew S.
Tu, Huakang
Hsu, Hil
Arbour, Kathryn C.
Awad, Mark M.
Riely, Gregory J.
Lovly, Christine M.
Anagnostou, Valsamo
author_facet Scharpf, Robert B.
Balan, Archana
Ricciuti, Biagio
Fiksel, Jacob
Cherry, Christopher
Wang, Chenguang
Lenoue-Newton, Michele L.
Rizvi, Hira A.
White, James R.
Baras, Alexander S.
Anaya, Jordan
Landon, Blair V.
Majcherska-Agrawal, Marta
Ghanem, Paola
Lee, Jocelyn
Raskin, Leon
Park, Andrew S.
Tu, Huakang
Hsu, Hil
Arbour, Kathryn C.
Awad, Mark M.
Riely, Gregory J.
Lovly, Christine M.
Anagnostou, Valsamo
author_sort Scharpf, Robert B.
collection PubMed
description The RAS family of small GTPases represents the most commonly activated oncogenes in human cancers. To better understand the prevalence of somatic RAS mutations and the compendium of genes that are coaltered in RAS-mutant tumors, we analyzed targeted next-generation sequencing data of 607,863 mutations from 66,372 tumors in 51 cancer types in the AACR Project GENIE Registry. Bayesian hierarchical models were implemented to estimate the cancer-specific prevalence of RAS and non-RAS somatic mutations, to evaluate co-occurrence and mutual exclusivity, and to model the effects of tumor mutation burden and mutational signatures on comutation patterns. These analyses revealed differential RAS prevalence and comutations with non-RAS genes in a cancer lineage-dependent and context-dependent manner, with differences across age, sex, and ethnic groups. Allele-specific RAS co-mutational patterns included an enrichment in NTRK3 and chromatin-regulating gene mutations in KRAS G12C-mutant non–small cell lung cancer. Integrated multiomic analyses of 10,217 tumors from The Cancer Genome Atlas (TCGA) revealed distinct genotype-driven gene expression programs pointing to differential recruitment of cancer hallmarks as well as phenotypic differences and immune surveillance states in the tumor microenvironment of RAS-mutant tumors. The distinct genomic tracks discovered in RAS-mutant tumors reflected differential clinical outcomes in TCGA cohort and in an independent cohort of patients with KRAS G12C-mutant non–small cell lung cancer that received immunotherapy-containing regimens. The RAS genetic architecture points to cancer lineage–specific therapeutic vulnerabilities that can be leveraged for rationally combining RAS-mutant allele-directed therapies with targeted therapies and immunotherapy. SIGNIFICANCE: The complex genomic landscape of RAS-mutant tumors is reflective of selection processes in a cancer lineage–specific and context-dependent manner, highlighting differential therapeutic vulnerabilities that can be clinically translated.
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spelling pubmed-96271272022-12-11 Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers Scharpf, Robert B. Balan, Archana Ricciuti, Biagio Fiksel, Jacob Cherry, Christopher Wang, Chenguang Lenoue-Newton, Michele L. Rizvi, Hira A. White, James R. Baras, Alexander S. Anaya, Jordan Landon, Blair V. Majcherska-Agrawal, Marta Ghanem, Paola Lee, Jocelyn Raskin, Leon Park, Andrew S. Tu, Huakang Hsu, Hil Arbour, Kathryn C. Awad, Mark M. Riely, Gregory J. Lovly, Christine M. Anagnostou, Valsamo Cancer Res Translational Science The RAS family of small GTPases represents the most commonly activated oncogenes in human cancers. To better understand the prevalence of somatic RAS mutations and the compendium of genes that are coaltered in RAS-mutant tumors, we analyzed targeted next-generation sequencing data of 607,863 mutations from 66,372 tumors in 51 cancer types in the AACR Project GENIE Registry. Bayesian hierarchical models were implemented to estimate the cancer-specific prevalence of RAS and non-RAS somatic mutations, to evaluate co-occurrence and mutual exclusivity, and to model the effects of tumor mutation burden and mutational signatures on comutation patterns. These analyses revealed differential RAS prevalence and comutations with non-RAS genes in a cancer lineage-dependent and context-dependent manner, with differences across age, sex, and ethnic groups. Allele-specific RAS co-mutational patterns included an enrichment in NTRK3 and chromatin-regulating gene mutations in KRAS G12C-mutant non–small cell lung cancer. Integrated multiomic analyses of 10,217 tumors from The Cancer Genome Atlas (TCGA) revealed distinct genotype-driven gene expression programs pointing to differential recruitment of cancer hallmarks as well as phenotypic differences and immune surveillance states in the tumor microenvironment of RAS-mutant tumors. The distinct genomic tracks discovered in RAS-mutant tumors reflected differential clinical outcomes in TCGA cohort and in an independent cohort of patients with KRAS G12C-mutant non–small cell lung cancer that received immunotherapy-containing regimens. The RAS genetic architecture points to cancer lineage–specific therapeutic vulnerabilities that can be leveraged for rationally combining RAS-mutant allele-directed therapies with targeted therapies and immunotherapy. SIGNIFICANCE: The complex genomic landscape of RAS-mutant tumors is reflective of selection processes in a cancer lineage–specific and context-dependent manner, highlighting differential therapeutic vulnerabilities that can be clinically translated. American Association for Cancer Research 2022-11-02 2022-09-08 /pmc/articles/PMC9627127/ /pubmed/36074020 http://dx.doi.org/10.1158/0008-5472.CAN-22-1731 Text en ©2022 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by-nc-nd/4.0/This open access article is distributed under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0) license.
spellingShingle Translational Science
Scharpf, Robert B.
Balan, Archana
Ricciuti, Biagio
Fiksel, Jacob
Cherry, Christopher
Wang, Chenguang
Lenoue-Newton, Michele L.
Rizvi, Hira A.
White, James R.
Baras, Alexander S.
Anaya, Jordan
Landon, Blair V.
Majcherska-Agrawal, Marta
Ghanem, Paola
Lee, Jocelyn
Raskin, Leon
Park, Andrew S.
Tu, Huakang
Hsu, Hil
Arbour, Kathryn C.
Awad, Mark M.
Riely, Gregory J.
Lovly, Christine M.
Anagnostou, Valsamo
Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers
title Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers
title_full Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers
title_fullStr Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers
title_full_unstemmed Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers
title_short Genomic Landscapes and Hallmarks of Mutant RAS in Human Cancers
title_sort genomic landscapes and hallmarks of mutant ras in human cancers
topic Translational Science
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9627127/
https://www.ncbi.nlm.nih.gov/pubmed/36074020
http://dx.doi.org/10.1158/0008-5472.CAN-22-1731
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