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Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities

BACKGROUND: Combined small-cell lung cancer (C-SCLC) is composed of SCLC admixed with a non-small-cell cancer component. They currently receive the same treatment as SCLC. The recent evidence that SCLC may belong to either of two lineages, neuroendocrine (NE) or non-NE, with different vulnerability...

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Autores principales: Simbolo, M., Centonze, G., Ali, G., Garzone, G., Taormina, S., Sabella, G., Ciaparrone, C., Mafficini, A., Grillo, F., Mangogna, A., Volante, M., Mastracci, L., Fontanini, G., Pilotto, S., Bria, E., Infante, M., Capella, C., Rolli, L., Pastorino, U., Milella, M., Milione, M., Scarpa, A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8695295/
https://www.ncbi.nlm.nih.gov/pubmed/34952268
http://dx.doi.org/10.1016/j.esmoop.2021.100308
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author Simbolo, M.
Centonze, G.
Ali, G.
Garzone, G.
Taormina, S.
Sabella, G.
Ciaparrone, C.
Mafficini, A.
Grillo, F.
Mangogna, A.
Volante, M.
Mastracci, L.
Fontanini, G.
Pilotto, S.
Bria, E.
Infante, M.
Capella, C.
Rolli, L.
Pastorino, U.
Milella, M.
Milione, M.
Scarpa, A.
author_facet Simbolo, M.
Centonze, G.
Ali, G.
Garzone, G.
Taormina, S.
Sabella, G.
Ciaparrone, C.
Mafficini, A.
Grillo, F.
Mangogna, A.
Volante, M.
Mastracci, L.
Fontanini, G.
Pilotto, S.
Bria, E.
Infante, M.
Capella, C.
Rolli, L.
Pastorino, U.
Milella, M.
Milione, M.
Scarpa, A.
author_sort Simbolo, M.
collection PubMed
description BACKGROUND: Combined small-cell lung cancer (C-SCLC) is composed of SCLC admixed with a non-small-cell cancer component. They currently receive the same treatment as SCLC. The recent evidence that SCLC may belong to either of two lineages, neuroendocrine (NE) or non-NE, with different vulnerability to specific cell death pathways such as ferroptosis, opens new therapeutic opportunities also for C-SCLC. MATERIALS AND METHODS: Thirteen C-SCLCs, including five with adenocarcinoma (CoADC), five with large-cell neuroendocrine carcinoma (CoLCNEC) and three with squamous cell carcinoma (CoSQC) components, were assessed for alterations in 409 genes and transcriptomic profiling of 20 815 genes. RESULTS: All 13 cases harbored TP53 (12 cases) and/or RB1 (7 cases) inactivation, which was accompanied by mutated KRAS in 4 and PTEN in 3 cases. Potentially targetable alterations included two KRAS G12C, two PIK3CA and one EGFR mutations. Comparison of C-SCLC transcriptomes with those of 57 pure histology lung cancers (17 ADCs, 20 SQCs, 11 LCNECs, 9 SCLCs) showed that CoLCNEC and CoADC constituted a standalone group of NE tumors, while CoSQC transcriptional setup was overlapping that of pure SQC. Using transcriptional signatures of NE versus non-NE SCLC as classifier, CoLCNEC was clearly NE while CoSQC was strongly non-NE and CoADC exhibited a heterogeneous phenotype. Similarly, using ferroptosis sensitivity/resistance markers, CoSQC was classified as sensitive (as expected for non-NE), CoLCNEC as resistant (as expected for NE) and CoADC showed a heterogeneous pattern. CONCLUSIONS: These data support routine molecular profiling of C-SCLC to search for targetable driver alterations and to precisely classify them according to therapeutically relevant subgroups (e.g. NE versus non-NE).
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spelling pubmed-86952952022-01-04 Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities Simbolo, M. Centonze, G. Ali, G. Garzone, G. Taormina, S. Sabella, G. Ciaparrone, C. Mafficini, A. Grillo, F. Mangogna, A. Volante, M. Mastracci, L. Fontanini, G. Pilotto, S. Bria, E. Infante, M. Capella, C. Rolli, L. Pastorino, U. Milella, M. Milione, M. Scarpa, A. ESMO Open Original Research BACKGROUND: Combined small-cell lung cancer (C-SCLC) is composed of SCLC admixed with a non-small-cell cancer component. They currently receive the same treatment as SCLC. The recent evidence that SCLC may belong to either of two lineages, neuroendocrine (NE) or non-NE, with different vulnerability to specific cell death pathways such as ferroptosis, opens new therapeutic opportunities also for C-SCLC. MATERIALS AND METHODS: Thirteen C-SCLCs, including five with adenocarcinoma (CoADC), five with large-cell neuroendocrine carcinoma (CoLCNEC) and three with squamous cell carcinoma (CoSQC) components, were assessed for alterations in 409 genes and transcriptomic profiling of 20 815 genes. RESULTS: All 13 cases harbored TP53 (12 cases) and/or RB1 (7 cases) inactivation, which was accompanied by mutated KRAS in 4 and PTEN in 3 cases. Potentially targetable alterations included two KRAS G12C, two PIK3CA and one EGFR mutations. Comparison of C-SCLC transcriptomes with those of 57 pure histology lung cancers (17 ADCs, 20 SQCs, 11 LCNECs, 9 SCLCs) showed that CoLCNEC and CoADC constituted a standalone group of NE tumors, while CoSQC transcriptional setup was overlapping that of pure SQC. Using transcriptional signatures of NE versus non-NE SCLC as classifier, CoLCNEC was clearly NE while CoSQC was strongly non-NE and CoADC exhibited a heterogeneous phenotype. Similarly, using ferroptosis sensitivity/resistance markers, CoSQC was classified as sensitive (as expected for non-NE), CoLCNEC as resistant (as expected for NE) and CoADC showed a heterogeneous pattern. CONCLUSIONS: These data support routine molecular profiling of C-SCLC to search for targetable driver alterations and to precisely classify them according to therapeutically relevant subgroups (e.g. NE versus non-NE). Elsevier 2021-12-21 /pmc/articles/PMC8695295/ /pubmed/34952268 http://dx.doi.org/10.1016/j.esmoop.2021.100308 Text en © 2021 The Author(s) 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 Research
Simbolo, M.
Centonze, G.
Ali, G.
Garzone, G.
Taormina, S.
Sabella, G.
Ciaparrone, C.
Mafficini, A.
Grillo, F.
Mangogna, A.
Volante, M.
Mastracci, L.
Fontanini, G.
Pilotto, S.
Bria, E.
Infante, M.
Capella, C.
Rolli, L.
Pastorino, U.
Milella, M.
Milione, M.
Scarpa, A.
Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities
title Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities
title_full Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities
title_fullStr Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities
title_full_unstemmed Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities
title_short Integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities
title_sort integrative molecular analysis of combined small-cell lung carcinomas identifies major subtypes with different therapeutic opportunities
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8695295/
https://www.ncbi.nlm.nih.gov/pubmed/34952268
http://dx.doi.org/10.1016/j.esmoop.2021.100308
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