EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures

SIMPLE SUMMARY: The phenotypic transition of tumor cells from epithelial to mesenchymal characteristics is called EMT and is widely discussed in the scientific community as a game changer in drug resistance and metastasis formation. However, clinical studies could not prove the efficacy of EMT-inter...

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Autores principales: Peindl, Matthias, Göttlich, Claudia, Crouch, Samantha, Hoff, Niklas, Lüttgens, Tamara, Schmitt, Franziska, Pereira, Jesús Guillermo Nieves, May, Celina, Schliermann, Anna, Kronenthaler, Corinna, Cheufou, Danjouma, Reu-Hofer, Simone, Rosenwald, Andreas, Weigl, Elena, Walles, Thorsten, Schüler, Julia, Dandekar, Thomas, Nietzer, Sarah, Dandekar, Gudrun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9099837/
https://www.ncbi.nlm.nih.gov/pubmed/35565305
http://dx.doi.org/10.3390/cancers14092176
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author Peindl, Matthias
Göttlich, Claudia
Crouch, Samantha
Hoff, Niklas
Lüttgens, Tamara
Schmitt, Franziska
Pereira, Jesús Guillermo Nieves
May, Celina
Schliermann, Anna
Kronenthaler, Corinna
Cheufou, Danjouma
Reu-Hofer, Simone
Rosenwald, Andreas
Weigl, Elena
Walles, Thorsten
Schüler, Julia
Dandekar, Thomas
Nietzer, Sarah
Dandekar, Gudrun
author_facet Peindl, Matthias
Göttlich, Claudia
Crouch, Samantha
Hoff, Niklas
Lüttgens, Tamara
Schmitt, Franziska
Pereira, Jesús Guillermo Nieves
May, Celina
Schliermann, Anna
Kronenthaler, Corinna
Cheufou, Danjouma
Reu-Hofer, Simone
Rosenwald, Andreas
Weigl, Elena
Walles, Thorsten
Schüler, Julia
Dandekar, Thomas
Nietzer, Sarah
Dandekar, Gudrun
author_sort Peindl, Matthias
collection PubMed
description SIMPLE SUMMARY: The phenotypic transition of tumor cells from epithelial to mesenchymal characteristics is called EMT and is widely discussed in the scientific community as a game changer in drug resistance and metastasis formation. However, clinical studies could not prove the efficacy of EMT-interfering treatments, and in clinical routine, EMT is not investigated to assess invasion. To fill this gap between bench and bedside, we use in this study a lung tumor tissue model with a preserved basement membrane for investigation of EMT functions with respect to invasion across this membrane and drug resistance. Our results suggest EMT is more a marker of drug resistance than a maker. Invasion is enhanced by EMT but more dependent on intrinsic factors, and EMT is not detected in the center of invasive tumor nodules. An in silico signaling network model is used to integrate these in vitro results and to reveal determinants for drug response. ABSTRACT: Epithelial-to-mesenchymal transition (EMT) is discussed to be centrally involved in invasion, stemness, and drug resistance. Experimental models to evaluate this process in its biological complexity are limited. To shed light on EMT impact and test drug response more reliably, we use a lung tumor test system based on a decellularized intestinal matrix showing more in vivo-like proliferation levels and enhanced expression of clinical markers and carcinogenesis-related genes. In our models, we found evidence for a correlation of EMT with drug resistance in primary and secondary resistant cells harboring KRAS(G12C) or EGFR mutations, which was simulated in silico based on an optimized signaling network topology. Notably, drug resistance did not correlate with EMT status in KRAS-mutated patient-derived xenograft (PDX) cell lines, and drug efficacy was not affected by EMT induction via TGF-β. To investigate further determinants of drug response, we tested several drugs in combination with a KRAS(G12C) inhibitor in KRAS(G12C) mutant HCC44 models, which, besides EMT, display mutations in P53, LKB1, KEAP1, and high c-MYC expression. We identified an aurora-kinase A (AURKA) inhibitor as the most promising candidate. In our network, AURKA is a centrally linked hub to EMT, proliferation, apoptosis, LKB1, and c-MYC. This exemplifies our systemic analysis approach for clinical translation of biomarker signatures.
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spelling pubmed-90998372022-05-14 EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures Peindl, Matthias Göttlich, Claudia Crouch, Samantha Hoff, Niklas Lüttgens, Tamara Schmitt, Franziska Pereira, Jesús Guillermo Nieves May, Celina Schliermann, Anna Kronenthaler, Corinna Cheufou, Danjouma Reu-Hofer, Simone Rosenwald, Andreas Weigl, Elena Walles, Thorsten Schüler, Julia Dandekar, Thomas Nietzer, Sarah Dandekar, Gudrun Cancers (Basel) Article SIMPLE SUMMARY: The phenotypic transition of tumor cells from epithelial to mesenchymal characteristics is called EMT and is widely discussed in the scientific community as a game changer in drug resistance and metastasis formation. However, clinical studies could not prove the efficacy of EMT-interfering treatments, and in clinical routine, EMT is not investigated to assess invasion. To fill this gap between bench and bedside, we use in this study a lung tumor tissue model with a preserved basement membrane for investigation of EMT functions with respect to invasion across this membrane and drug resistance. Our results suggest EMT is more a marker of drug resistance than a maker. Invasion is enhanced by EMT but more dependent on intrinsic factors, and EMT is not detected in the center of invasive tumor nodules. An in silico signaling network model is used to integrate these in vitro results and to reveal determinants for drug response. ABSTRACT: Epithelial-to-mesenchymal transition (EMT) is discussed to be centrally involved in invasion, stemness, and drug resistance. Experimental models to evaluate this process in its biological complexity are limited. To shed light on EMT impact and test drug response more reliably, we use a lung tumor test system based on a decellularized intestinal matrix showing more in vivo-like proliferation levels and enhanced expression of clinical markers and carcinogenesis-related genes. In our models, we found evidence for a correlation of EMT with drug resistance in primary and secondary resistant cells harboring KRAS(G12C) or EGFR mutations, which was simulated in silico based on an optimized signaling network topology. Notably, drug resistance did not correlate with EMT status in KRAS-mutated patient-derived xenograft (PDX) cell lines, and drug efficacy was not affected by EMT induction via TGF-β. To investigate further determinants of drug response, we tested several drugs in combination with a KRAS(G12C) inhibitor in KRAS(G12C) mutant HCC44 models, which, besides EMT, display mutations in P53, LKB1, KEAP1, and high c-MYC expression. We identified an aurora-kinase A (AURKA) inhibitor as the most promising candidate. In our network, AURKA is a centrally linked hub to EMT, proliferation, apoptosis, LKB1, and c-MYC. This exemplifies our systemic analysis approach for clinical translation of biomarker signatures. MDPI 2022-04-27 /pmc/articles/PMC9099837/ /pubmed/35565305 http://dx.doi.org/10.3390/cancers14092176 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Peindl, Matthias
Göttlich, Claudia
Crouch, Samantha
Hoff, Niklas
Lüttgens, Tamara
Schmitt, Franziska
Pereira, Jesús Guillermo Nieves
May, Celina
Schliermann, Anna
Kronenthaler, Corinna
Cheufou, Danjouma
Reu-Hofer, Simone
Rosenwald, Andreas
Weigl, Elena
Walles, Thorsten
Schüler, Julia
Dandekar, Thomas
Nietzer, Sarah
Dandekar, Gudrun
EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures
title EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures
title_full EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures
title_fullStr EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures
title_full_unstemmed EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures
title_short EMT, Stemness, and Drug Resistance in Biological Context: A 3D Tumor Tissue/In Silico Platform for Analysis of Combinatorial Treatment in NSCLC with Aggressive KRAS-Biomarker Signatures
title_sort emt, stemness, and drug resistance in biological context: a 3d tumor tissue/in silico platform for analysis of combinatorial treatment in nsclc with aggressive kras-biomarker signatures
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9099837/
https://www.ncbi.nlm.nih.gov/pubmed/35565305
http://dx.doi.org/10.3390/cancers14092176
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