Establishment and genomic characterization of the new chordoma cell line Chor-IN-1

Abstract Chordomas are rare, slowly growing tumors with high medical need, arising in the axial skeleton from notochord remnants. The transcription factor “brachyury” represents a distinctive molecular marker and a key oncogenic driver of chordomas. Tyrosine kinase receptors are also expressed, but...

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Main Authors: Roberta Bosotti, Paola Magnaghi, Sebastiano Di Bella, Liviana Cozzi, Carlo Cusi, Fabio Bozzi, Nicola Beltrami, Giovanni Carapezza, Dario Ballinari, Nadia Amboldi, Rosita Lupi, Alessio Somaschini, Laura Raddrizzani, Barbara Salom, Arturo Galvani, Silvia Stacchiotti, Elena Tamborini, Antonella Isacchi
Format: Article
Language:English
Published: Nature Publishing Group 2017-08-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-017-10044-3
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spelling doaj-2e2d8fd735034e6896516334379601fa2020-12-08T00:46:39ZengNature Publishing GroupScientific Reports2045-23222017-08-017111410.1038/s41598-017-10044-3Establishment and genomic characterization of the new chordoma cell line Chor-IN-1Roberta Bosotti0Paola Magnaghi1Sebastiano Di Bella2Liviana Cozzi3Carlo Cusi4Fabio Bozzi5Nicola Beltrami6Giovanni Carapezza7Dario Ballinari8Nadia Amboldi9Rosita Lupi10Alessio Somaschini11Laura Raddrizzani12Barbara Salom13Arturo Galvani14Silvia Stacchiotti15Elena Tamborini16Antonella Isacchi17Oncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesFondazione IRCCS Istituto Nazionale dei TumoriL.C. Laboratori CampisiOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesOncology, Nerviano Medical SciencesFondazione IRCCS Istituto Nazionale dei TumoriFondazione IRCCS Istituto Nazionale dei TumoriOncology, Nerviano Medical SciencesAbstract Chordomas are rare, slowly growing tumors with high medical need, arising in the axial skeleton from notochord remnants. The transcription factor “brachyury” represents a distinctive molecular marker and a key oncogenic driver of chordomas. Tyrosine kinase receptors are also expressed, but so far kinase inhibitors have not shown clear clinical efficacy in chordoma patients. The need for effective therapies is extremely high, but the paucity of established chordoma cell lines has limited preclinical research. Here we describe the isolation of the new Chor-IN-1 cell line from a recurrent sacral chordoma and its characterization as compared to other chordoma cell lines. Chor-IN-1 displays genomic identity to the tumor of origin and has morphological features, growth characteristics and chromosomal abnormalities typical of chordoma, with expression of brachyury and other relevant biomarkers. Chor-IN-1 gene variants, copy number alterations and kinome gene expression were analyzed in comparison to other four chordoma cell lines, generating large scale DNA and mRNA genomic data that can be exploited for the identification of novel pharmacological targets and candidate predictive biomarkers of drug sensitivity in chordoma. The establishment of this new, well characterized chordoma cell line provides a useful tool for the identification of drugs active in chordoma.https://doi.org/10.1038/s41598-017-10044-3
collection DOAJ
language English
format Article
sources DOAJ
author Roberta Bosotti
Paola Magnaghi
Sebastiano Di Bella
Liviana Cozzi
Carlo Cusi
Fabio Bozzi
Nicola Beltrami
Giovanni Carapezza
Dario Ballinari
Nadia Amboldi
Rosita Lupi
Alessio Somaschini
Laura Raddrizzani
Barbara Salom
Arturo Galvani
Silvia Stacchiotti
Elena Tamborini
Antonella Isacchi
spellingShingle Roberta Bosotti
Paola Magnaghi
Sebastiano Di Bella
Liviana Cozzi
Carlo Cusi
Fabio Bozzi
Nicola Beltrami
Giovanni Carapezza
Dario Ballinari
Nadia Amboldi
Rosita Lupi
Alessio Somaschini
Laura Raddrizzani
Barbara Salom
Arturo Galvani
Silvia Stacchiotti
Elena Tamborini
Antonella Isacchi
Establishment and genomic characterization of the new chordoma cell line Chor-IN-1
Scientific Reports
author_facet Roberta Bosotti
Paola Magnaghi
Sebastiano Di Bella
Liviana Cozzi
Carlo Cusi
Fabio Bozzi
Nicola Beltrami
Giovanni Carapezza
Dario Ballinari
Nadia Amboldi
Rosita Lupi
Alessio Somaschini
Laura Raddrizzani
Barbara Salom
Arturo Galvani
Silvia Stacchiotti
Elena Tamborini
Antonella Isacchi
author_sort Roberta Bosotti
title Establishment and genomic characterization of the new chordoma cell line Chor-IN-1
title_short Establishment and genomic characterization of the new chordoma cell line Chor-IN-1
title_full Establishment and genomic characterization of the new chordoma cell line Chor-IN-1
title_fullStr Establishment and genomic characterization of the new chordoma cell line Chor-IN-1
title_full_unstemmed Establishment and genomic characterization of the new chordoma cell line Chor-IN-1
title_sort establishment and genomic characterization of the new chordoma cell line chor-in-1
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2017-08-01
description Abstract Chordomas are rare, slowly growing tumors with high medical need, arising in the axial skeleton from notochord remnants. The transcription factor “brachyury” represents a distinctive molecular marker and a key oncogenic driver of chordomas. Tyrosine kinase receptors are also expressed, but so far kinase inhibitors have not shown clear clinical efficacy in chordoma patients. The need for effective therapies is extremely high, but the paucity of established chordoma cell lines has limited preclinical research. Here we describe the isolation of the new Chor-IN-1 cell line from a recurrent sacral chordoma and its characterization as compared to other chordoma cell lines. Chor-IN-1 displays genomic identity to the tumor of origin and has morphological features, growth characteristics and chromosomal abnormalities typical of chordoma, with expression of brachyury and other relevant biomarkers. Chor-IN-1 gene variants, copy number alterations and kinome gene expression were analyzed in comparison to other four chordoma cell lines, generating large scale DNA and mRNA genomic data that can be exploited for the identification of novel pharmacological targets and candidate predictive biomarkers of drug sensitivity in chordoma. The establishment of this new, well characterized chordoma cell line provides a useful tool for the identification of drugs active in chordoma.
url https://doi.org/10.1038/s41598-017-10044-3
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