Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers

Pancreatic cancer is an increasing cause of cancer related death worldwide. KRAS is the dominant oncogene in this cancer type and molecular rationale would indicate, that inhibitors of the downstream target MEK could be appropriate targeted agents, but clinical trials have failed so far to achieve s...

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Autores principales: Brauswetter, Diána, Gurbi, Bianka, Varga, Attila, Várkondi, Edit, Schwab, Richárd, Bánhegyi, Gábor, Fábián, Orsolya, Kéri, György, Vályi-Nagy, István, Peták, István
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5619833/
https://www.ncbi.nlm.nih.gov/pubmed/28957417
http://dx.doi.org/10.1371/journal.pone.0185687
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author Brauswetter, Diána
Gurbi, Bianka
Varga, Attila
Várkondi, Edit
Schwab, Richárd
Bánhegyi, Gábor
Fábián, Orsolya
Kéri, György
Vályi-Nagy, István
Peták, István
author_facet Brauswetter, Diána
Gurbi, Bianka
Varga, Attila
Várkondi, Edit
Schwab, Richárd
Bánhegyi, Gábor
Fábián, Orsolya
Kéri, György
Vályi-Nagy, István
Peták, István
author_sort Brauswetter, Diána
collection PubMed
description Pancreatic cancer is an increasing cause of cancer related death worldwide. KRAS is the dominant oncogene in this cancer type and molecular rationale would indicate, that inhibitors of the downstream target MEK could be appropriate targeted agents, but clinical trials have failed so far to achieve statistically significant benefit in unselected patients. We aimed to identify predictive molecular biomarkers that can help to define subgroups where MEK inhibitors might be beneficial alone or in combination. Next-generation sequencing data of 50 genes in three pancreatic cancer cell lines (MiaPaCa2, BxPC3 and Panc1) were analyzed and compared to the molecular profile of 138 clinical pancreatic cancer samples to identify the molecular subtypes of pancreatic cancer these cell lines represent. Luminescent cell viability assay was used to determine the sensitivity of cell lines to kinase inhibitors. Western blot was used to analyze the pathway activity of the examined cell lines. According to our cell viability and pathway activity data on these model cell lines only cells harboring the rare G12C KRAS mutation and low EGFR expression are sensitive to single MEK inhibitor (trametinib) treatment. The common G12D KRAS mutation leads to elevated baseline Akt activity, thus treatment with single MEK inhibitors fails. However, combination of MEK and Akt inhibitors are synergistic in this case. In case of wild-type KRAS and high EGFR expression MEK inhibitor induced Akt phosphorylation leads to trametinib resistance which necessitates for MEK and EGFR or Akt inhibitor combination treatment. In all we provide strong preclinical rational and possible molecular mechanism to revisit MEK inhibitor therapy in pancreatic cancer in both monotherapy and combination, based on molecular profile analysis of pancreatic cancer samples and cell lines. According to our most remarkable finding, a small subgroup of patients with G12C KRAS mutation may still benefit from MEK inhibitor monotherapy.
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spelling pubmed-56198332017-10-17 Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers Brauswetter, Diána Gurbi, Bianka Varga, Attila Várkondi, Edit Schwab, Richárd Bánhegyi, Gábor Fábián, Orsolya Kéri, György Vályi-Nagy, István Peták, István PLoS One Research Article Pancreatic cancer is an increasing cause of cancer related death worldwide. KRAS is the dominant oncogene in this cancer type and molecular rationale would indicate, that inhibitors of the downstream target MEK could be appropriate targeted agents, but clinical trials have failed so far to achieve statistically significant benefit in unselected patients. We aimed to identify predictive molecular biomarkers that can help to define subgroups where MEK inhibitors might be beneficial alone or in combination. Next-generation sequencing data of 50 genes in three pancreatic cancer cell lines (MiaPaCa2, BxPC3 and Panc1) were analyzed and compared to the molecular profile of 138 clinical pancreatic cancer samples to identify the molecular subtypes of pancreatic cancer these cell lines represent. Luminescent cell viability assay was used to determine the sensitivity of cell lines to kinase inhibitors. Western blot was used to analyze the pathway activity of the examined cell lines. According to our cell viability and pathway activity data on these model cell lines only cells harboring the rare G12C KRAS mutation and low EGFR expression are sensitive to single MEK inhibitor (trametinib) treatment. The common G12D KRAS mutation leads to elevated baseline Akt activity, thus treatment with single MEK inhibitors fails. However, combination of MEK and Akt inhibitors are synergistic in this case. In case of wild-type KRAS and high EGFR expression MEK inhibitor induced Akt phosphorylation leads to trametinib resistance which necessitates for MEK and EGFR or Akt inhibitor combination treatment. In all we provide strong preclinical rational and possible molecular mechanism to revisit MEK inhibitor therapy in pancreatic cancer in both monotherapy and combination, based on molecular profile analysis of pancreatic cancer samples and cell lines. According to our most remarkable finding, a small subgroup of patients with G12C KRAS mutation may still benefit from MEK inhibitor monotherapy. Public Library of Science 2017-09-28 /pmc/articles/PMC5619833/ /pubmed/28957417 http://dx.doi.org/10.1371/journal.pone.0185687 Text en © 2017 Brauswetter et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Brauswetter, Diána
Gurbi, Bianka
Varga, Attila
Várkondi, Edit
Schwab, Richárd
Bánhegyi, Gábor
Fábián, Orsolya
Kéri, György
Vályi-Nagy, István
Peták, István
Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers
title Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers
title_full Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers
title_fullStr Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers
title_full_unstemmed Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers
title_short Molecular subtype specific efficacy of MEK inhibitors in pancreatic cancers
title_sort molecular subtype specific efficacy of mek inhibitors in pancreatic cancers
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5619833/
https://www.ncbi.nlm.nih.gov/pubmed/28957417
http://dx.doi.org/10.1371/journal.pone.0185687
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