Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing

INTRODUCTION: Genomic alterations in the juxtamembrane exon 14 splice sites in NSCLC lead to increased MET stability and oncogenesis. We present the largest cohort study of MET Exon 14 (METex14) using whole transcriptome sequencing. METHODS: A total of 21,582 NSCLC tumor samples underwent complete g...

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Autores principales: Kim, So Yeon, Yin, Jun, Bohlman, Stephen, Walker, Phillip, Dacic, Sanja, Kim, Chul, Khan, Hina, Liu, Stephen V., Ma, Patrick C., Nagasaka, Misako, Reckamp, Karen L., Abraham, Jim, Uprety, Dipesh, Wang, Feng, Xiu, Joanne, Zhang, Jian, Cheng, Haiying, Halmos, Balazs
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9445394/
https://www.ncbi.nlm.nih.gov/pubmed/36082279
http://dx.doi.org/10.1016/j.jtocrr.2022.100381
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author Kim, So Yeon
Yin, Jun
Bohlman, Stephen
Walker, Phillip
Dacic, Sanja
Kim, Chul
Khan, Hina
Liu, Stephen V.
Ma, Patrick C.
Nagasaka, Misako
Reckamp, Karen L.
Abraham, Jim
Uprety, Dipesh
Wang, Feng
Xiu, Joanne
Zhang, Jian
Cheng, Haiying
Halmos, Balazs
author_facet Kim, So Yeon
Yin, Jun
Bohlman, Stephen
Walker, Phillip
Dacic, Sanja
Kim, Chul
Khan, Hina
Liu, Stephen V.
Ma, Patrick C.
Nagasaka, Misako
Reckamp, Karen L.
Abraham, Jim
Uprety, Dipesh
Wang, Feng
Xiu, Joanne
Zhang, Jian
Cheng, Haiying
Halmos, Balazs
author_sort Kim, So Yeon
collection PubMed
description INTRODUCTION: Genomic alterations in the juxtamembrane exon 14 splice sites in NSCLC lead to increased MET stability and oncogenesis. We present the largest cohort study of MET Exon 14 (METex14) using whole transcriptome sequencing. METHODS: A total of 21,582 NSCLC tumor samples underwent complete genomic profiling with next-generation sequencing of DNA (592 Gene Panel, NextSeq, whole exome sequencing, NovaSeq) and RNA (NovaSeq, whole transcriptome sequencing). Clinicopathologic information including programmed death-ligand 1 and tumor mutational burden were collected and RNA expression for mutation subtypes and MET amplification were quantified. Immunogenic signatures and potential pathways of invasion were characterized using single-sample gene set enrichment analysis and mRNA gene signatures. RESULTS: A total of 533tumors (2.47%) with METex14 were identified. The most common alterations were point mutations (49.5%) at donor splice sites. Most alterations translated to increased MET expression, with MET co-amplification resulting in synergistic increase in expression (q < 0.05). Common coalterations were amplifications of MDM2 (19.0% versus 1.8% wild-type [WT]), HMGA2 (13.2% versus 0.98% WT), and CDK4 (10.0% versus 1.5% WT) (q < 0.05). High programmed death-ligand 1 > 50% (52.5% versus 27.3% WT, q < 0.0001) and lower proportion of high tumor mutational burden (>10 mutations per megabase, 8.3% versus 36.7% WT, p < 0.0001) were associated with METex14, which were also enriched in both immunogenic signatures and immunosuppressive checkpoints. Pathways associated with METex14 included angiogenesis and apical junction pathways (q < 0.05). CONCLUSIONS: METex14 splicing alterations and MET co-amplification translated to higher and synergistic MET expression at the transcriptomic level. High frequencies of MDM2 and CDK4 co-amplifications and association with multiple immunosuppressive checkpoints and angiogenic pathways provide insight into potential actionable targets for combination strategies in METex14 NSCLC.
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spelling pubmed-94453942022-09-07 Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing Kim, So Yeon Yin, Jun Bohlman, Stephen Walker, Phillip Dacic, Sanja Kim, Chul Khan, Hina Liu, Stephen V. Ma, Patrick C. Nagasaka, Misako Reckamp, Karen L. Abraham, Jim Uprety, Dipesh Wang, Feng Xiu, Joanne Zhang, Jian Cheng, Haiying Halmos, Balazs JTO Clin Res Rep Original Article INTRODUCTION: Genomic alterations in the juxtamembrane exon 14 splice sites in NSCLC lead to increased MET stability and oncogenesis. We present the largest cohort study of MET Exon 14 (METex14) using whole transcriptome sequencing. METHODS: A total of 21,582 NSCLC tumor samples underwent complete genomic profiling with next-generation sequencing of DNA (592 Gene Panel, NextSeq, whole exome sequencing, NovaSeq) and RNA (NovaSeq, whole transcriptome sequencing). Clinicopathologic information including programmed death-ligand 1 and tumor mutational burden were collected and RNA expression for mutation subtypes and MET amplification were quantified. Immunogenic signatures and potential pathways of invasion were characterized using single-sample gene set enrichment analysis and mRNA gene signatures. RESULTS: A total of 533tumors (2.47%) with METex14 were identified. The most common alterations were point mutations (49.5%) at donor splice sites. Most alterations translated to increased MET expression, with MET co-amplification resulting in synergistic increase in expression (q < 0.05). Common coalterations were amplifications of MDM2 (19.0% versus 1.8% wild-type [WT]), HMGA2 (13.2% versus 0.98% WT), and CDK4 (10.0% versus 1.5% WT) (q < 0.05). High programmed death-ligand 1 > 50% (52.5% versus 27.3% WT, q < 0.0001) and lower proportion of high tumor mutational burden (>10 mutations per megabase, 8.3% versus 36.7% WT, p < 0.0001) were associated with METex14, which were also enriched in both immunogenic signatures and immunosuppressive checkpoints. Pathways associated with METex14 included angiogenesis and apical junction pathways (q < 0.05). CONCLUSIONS: METex14 splicing alterations and MET co-amplification translated to higher and synergistic MET expression at the transcriptomic level. High frequencies of MDM2 and CDK4 co-amplifications and association with multiple immunosuppressive checkpoints and angiogenic pathways provide insight into potential actionable targets for combination strategies in METex14 NSCLC. Elsevier 2022-07-22 /pmc/articles/PMC9445394/ /pubmed/36082279 http://dx.doi.org/10.1016/j.jtocrr.2022.100381 Text en © 2022 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
Kim, So Yeon
Yin, Jun
Bohlman, Stephen
Walker, Phillip
Dacic, Sanja
Kim, Chul
Khan, Hina
Liu, Stephen V.
Ma, Patrick C.
Nagasaka, Misako
Reckamp, Karen L.
Abraham, Jim
Uprety, Dipesh
Wang, Feng
Xiu, Joanne
Zhang, Jian
Cheng, Haiying
Halmos, Balazs
Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing
title Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing
title_full Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing
title_fullStr Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing
title_full_unstemmed Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing
title_short Characterization of MET Exon 14 Skipping Alterations (in NSCLC) and Identification of Potential Therapeutic Targets Using Whole Transcriptome Sequencing
title_sort characterization of met exon 14 skipping alterations (in nsclc) and identification of potential therapeutic targets using whole transcriptome sequencing
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9445394/
https://www.ncbi.nlm.nih.gov/pubmed/36082279
http://dx.doi.org/10.1016/j.jtocrr.2022.100381
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