EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen

Chordoma is a rare malignant bone tumour with a poor prognosis and limited therapeutic options. We undertook a focused compound screen (FCS) against 1097 compounds on three well‐characterized chordoma cell lines; 154 compounds were selected from the single concentration screen (1 µm), based on their...

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Autores principales: Scheipl, Susanne, Barnard, Michelle, Cottone, Lucia, Jorgensen, Mette, Drewry, David H, Zuercher, William J, Turlais, Fabrice, Ye, Hongtao, Leite, Ana P, Smith, James A, Leithner, Andreas, Möller, Peter, Brüderlein, Silke, Guppy, Naomi, Amary, Fernanda, Tirabosco, Roberto, Strauss, Sandra J, Pillay, Nischalan, Flanagan, Adrienne M
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Ltd 2016
Materias:
Original Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4922416/
https://www.ncbi.nlm.nih.gov/pubmed/27102572
http://dx.doi.org/10.1002/path.4729
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author Scheipl, Susanne
Barnard, Michelle
Cottone, Lucia
Jorgensen, Mette
Drewry, David H
Zuercher, William J
Turlais, Fabrice
Ye, Hongtao
Leite, Ana P
Smith, James A
Leithner, Andreas
Möller, Peter
Brüderlein, Silke
Guppy, Naomi
Amary, Fernanda
Tirabosco, Roberto
Strauss, Sandra J
Pillay, Nischalan
Flanagan, Adrienne M
author_facet Scheipl, Susanne
Barnard, Michelle
Cottone, Lucia
Jorgensen, Mette
Drewry, David H
Zuercher, William J
Turlais, Fabrice
Ye, Hongtao
Leite, Ana P
Smith, James A
Leithner, Andreas
Möller, Peter
Brüderlein, Silke
Guppy, Naomi
Amary, Fernanda
Tirabosco, Roberto
Strauss, Sandra J
Pillay, Nischalan
Flanagan, Adrienne M
author_sort Scheipl, Susanne
collection PubMed
description Chordoma is a rare malignant bone tumour with a poor prognosis and limited therapeutic options. We undertook a focused compound screen (FCS) against 1097 compounds on three well‐characterized chordoma cell lines; 154 compounds were selected from the single concentration screen (1 µm), based on their growth‐inhibitory effect. Their half‐maximal effective concentration (EC(50)) values were determined in chordoma cells and normal fibroblasts. Twenty‐seven of these compounds displayed chordoma selective cell kill and 21/27 (78%) were found to be EGFR/ERBB family inhibitors. EGFR inhibitors in clinical development were then studied on an extended cell line panel of seven chordoma cell lines, four of which were sensitive to EGFR inhibition. Sapitinib (AstraZeneca) emerged as the lead compound, followed by gefitinib (AstraZeneca) and erlotinib (Roche/Genentech). The compounds were shown to induce apoptosis in the sensitive cell lines and suppressed phospho‐EGFR and its downstream pathways in a dose‐dependent manner. Analysis of substituent patterns suggested that EGFR‐inhibitors with small aniline substituents in the 4‐position of the quinazoline ring were more effective than inhibitors with large substituents in that position. Sapitinib showed significantly reduced tumour growth in two xenograft mouse models (U‐CH1 xenograft and a patient‐derived xenograft, SF8894). One of the resistant cell lines (U‐CH2) was shown to express high levels of phospho‐MET, a known bypass signalling pathway to EGFR. Neither amplifications (EGFR, ERBB2, MET) nor mutations in EGFR, ERBB2, ERBB4, PIK3CA, BRAF, NRAS, KRAS, PTEN, MET or other cancer gene hotspots were detected in the cell lines. Our findings are consistent with the reported (p‐)EGFR expression in the majority of clinical samples, and provide evidence for exploring the efficacy of EGFR inhibitors in the treatment of patients with chordoma and studying possible resistance mechanisms to these compounds in vitro and in vivo. © 2016 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.
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spelling pubmed-49224162016-07-19 EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen Scheipl, Susanne Barnard, Michelle Cottone, Lucia Jorgensen, Mette Drewry, David H Zuercher, William J Turlais, Fabrice Ye, Hongtao Leite, Ana P Smith, James A Leithner, Andreas Möller, Peter Brüderlein, Silke Guppy, Naomi Amary, Fernanda Tirabosco, Roberto Strauss, Sandra J Pillay, Nischalan Flanagan, Adrienne M J Pathol Original Papers Chordoma is a rare malignant bone tumour with a poor prognosis and limited therapeutic options. We undertook a focused compound screen (FCS) against 1097 compounds on three well‐characterized chordoma cell lines; 154 compounds were selected from the single concentration screen (1 µm), based on their growth‐inhibitory effect. Their half‐maximal effective concentration (EC(50)) values were determined in chordoma cells and normal fibroblasts. Twenty‐seven of these compounds displayed chordoma selective cell kill and 21/27 (78%) were found to be EGFR/ERBB family inhibitors. EGFR inhibitors in clinical development were then studied on an extended cell line panel of seven chordoma cell lines, four of which were sensitive to EGFR inhibition. Sapitinib (AstraZeneca) emerged as the lead compound, followed by gefitinib (AstraZeneca) and erlotinib (Roche/Genentech). The compounds were shown to induce apoptosis in the sensitive cell lines and suppressed phospho‐EGFR and its downstream pathways in a dose‐dependent manner. Analysis of substituent patterns suggested that EGFR‐inhibitors with small aniline substituents in the 4‐position of the quinazoline ring were more effective than inhibitors with large substituents in that position. Sapitinib showed significantly reduced tumour growth in two xenograft mouse models (U‐CH1 xenograft and a patient‐derived xenograft, SF8894). One of the resistant cell lines (U‐CH2) was shown to express high levels of phospho‐MET, a known bypass signalling pathway to EGFR. Neither amplifications (EGFR, ERBB2, MET) nor mutations in EGFR, ERBB2, ERBB4, PIK3CA, BRAF, NRAS, KRAS, PTEN, MET or other cancer gene hotspots were detected in the cell lines. Our findings are consistent with the reported (p‐)EGFR expression in the majority of clinical samples, and provide evidence for exploring the efficacy of EGFR inhibitors in the treatment of patients with chordoma and studying possible resistance mechanisms to these compounds in vitro and in vivo. © 2016 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland. John Wiley & Sons, Ltd 2016-05-31 2016-07 /pmc/articles/PMC4922416/ /pubmed/27102572 http://dx.doi.org/10.1002/path.4729 Text en © 2016 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland. This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Papers
Scheipl, Susanne
Barnard, Michelle
Cottone, Lucia
Jorgensen, Mette
Drewry, David H
Zuercher, William J
Turlais, Fabrice
Ye, Hongtao
Leite, Ana P
Smith, James A
Leithner, Andreas
Möller, Peter
Brüderlein, Silke
Guppy, Naomi
Amary, Fernanda
Tirabosco, Roberto
Strauss, Sandra J
Pillay, Nischalan
Flanagan, Adrienne M
EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen
title EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen
title_full EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen
title_fullStr EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen
title_full_unstemmed EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen
title_short EGFR inhibitors identified as a potential treatment for chordoma in a focused compound screen
title_sort egfr inhibitors identified as a potential treatment for chordoma in a focused compound screen
topic Original Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4922416/
https://www.ncbi.nlm.nih.gov/pubmed/27102572
http://dx.doi.org/10.1002/path.4729
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