Selective treatment pressure in colon cancer drives the molecular profile of resistant circulating tumor cell clones

The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastati...

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Published in	Molecular cancer Vol. 20; no. 1; pp. 30 - 6
Main Authors	Cayrefourcq, Laure, Thomas, Frédéric, Mazard, Thibault, Assenat, Eric, Assou, Said, Alix-Panabières, Catherine
Format	Journal Article
Language	English
Published	England BioMed Central Ltd 08.02.2021 BioMed Central BMC
Subjects	1-Phosphatidylinositol 3-kinase 5-Fluorouracil AKT protein ALDOB Biochemistry, Molecular Biology Biomarkers Biomarkers, Tumor Biopsy Cancer Cancer therapies CDA Chemotherapy Circulating tumor cells Clonal evolution Cloning Colon cancer Colonic Neoplasms Colonic Neoplasms - genetics Colonic Neoplasms - pathology Colonic Neoplasms - therapy Colorectal cancer Computational Biology Computational Biology - methods Cytidine deaminase Detoxification Development and progression Drug resistance Drug Resistance, Neoplasm Drug Resistance, Neoplasm - drug effects Drug therapy Energy metabolism Enzymes Gene expression Gene Expression Profiling Genes Genomics Human health and pathology Humans Hépatology and Gastroenterology Letter to the Editor Life Sciences Liver Liver Neoplasms Liver Neoplasms - metabolism Liver Neoplasms - secondary Metabolism Metastases Metastasis Neoplasm Metastasis Neoplasm Staging Neoplastic Cells, Circulating Neoplastic Cells, Circulating - drug effects Neoplastic Cells, Circulating - metabolism Neoplastic Cells, Circulating - pathology Patients Peripheral blood Physiological aspects Precision medicine Stem cells TOR protein Transcriptome Tumor cells Tumors Xenobiotics Clonal evolution CDA Colon cancer ALDOB Circulating tumor cells Gene expression
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Abstract	The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were ( i ) to compare the gene expression profiles of these CTC lines, and ( ii ) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote ( i ) drug resistance, ( ii ) xenobiotic and energy metabolism, and ( iii ) stem cell properties and plasticity.
AbstractList	The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were (i) to compare the gene expression profiles of these CTC lines, and (ii) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote (i) drug resistance, (ii) xenobiotic and energy metabolism, and (iii) stem cell properties and plasticity. The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were (i) to compare the gene expression profiles of these CTC lines, and (ii) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote (i) drug resistance, (ii) xenobiotic and energy metabolism, and (iii) stem cell properties and plasticity.The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were (i) to compare the gene expression profiles of these CTC lines, and (ii) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote (i) drug resistance, (ii) xenobiotic and energy metabolism, and (iii) stem cell properties and plasticity. Abstract The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were (i) to compare the gene expression profiles of these CTC lines, and (ii) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote (i) drug resistance, (ii) xenobiotic and energy metabolism, and (iii) stem cell properties and plasticity. The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were ( i ) to compare the gene expression profiles of these CTC lines, and ( ii ) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote ( i ) drug resistance, ( ii ) xenobiotic and energy metabolism, and ( iii ) stem cell properties and plasticity. The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were ( ) to compare the gene expression profiles of these CTC lines, and ( ) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote ( ) drug resistance, ( ) xenobiotic and energy metabolism, and ( ) stem cell properties and plasticity. The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of treatment efficacy. We established the first and still only nine permanent colon CTC lines from peripheral blood samples of a patient with metastatic colon cancer collected at different time points during treatment and cancer progression. The study objectives were (i) to compare the gene expression profiles of these CTC lines, and (ii) to determine the main features acquired during treatment. The number of upregulated genes was higher in the CTC lines obtained after treatment, indicating that they acquired properties to escape treatment pressure. Among these upregulated genes, some are involved in the mTOR and PI3K/AKT signaling pathways. Moreover, cytidine deaminase expression was significantly increased in the CTC lines obtained after failure of the first- and second-line 5-fluorouracile-based treatments, suggesting that these CTCs can eliminate this specific drug and resist to therapy. Several enzymes involved in xenobiotic metabolism also were upregulated after treatment, suggesting the activation of detoxification mechanisms in response to chemotherapy. Finally, the significant higher expression of aldolase B in four of the six CTC lines obtained after treatment withdrawal and cancer progression indicated that these clones originated from liver metastases. In conclusion, these CTC lines generated at different time points during treatment of metastatic colon cancer in a single patient are characterized by the deregulation of different genes that promote (i) drug resistance, (ii) xenobiotic and energy metabolism, and (iii) stem cell properties and plasticity. Keywords: Circulating tumor cells, Gene expression, Clonal evolution, Colon cancer, CDA, ALDOB
ArticleNumber	30
Audience	Academic
Author	Mazard, Thibault Cayrefourcq, Laure Assou, Said Alix-Panabières, Catherine Assenat, Eric Thomas, Frédéric
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Cites_doi	10.1038/s41598-018-34365-z 10.15252/emmm.201911908 10.1200/JCO.2008.18.6544 10.1038/d41586-020-00844-5 10.1073/pnas.1612229114 10.1016/j.cmet.2018.04.003 10.1038/s41571-019-0187-3 10.2147/OTT.S110203 10.1159/000477484 10.1373/clinchem.2016.263582 10.1016/j.neo.2017.05.002 10.1038/onc.2013.357 10.1186/s12943-015-0437-7 10.1097/00007611-199301000-00009 10.1016/j.mam.2019.07.008 10.1158/0008-5472.CAN-14-2613 10.2174/1389450120666190618123846 10.3390/cells9092129
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Keywords	Clonal evolution CDA Colon cancer ALDOB Circulating tumor cells Gene expression
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References	C Peitzsch (1326_CR11) 2020; S1044-579X A Soler (1326_CR6) 2018; 8 A Narayanankutty (1326_CR9) 2019; 20 DS Chandrashekar (1326_CR14) 2017; 19 V Patanaphan (1326_CR18) 1993; 86 C Koch (1326_CR3) 2020; 12 C Alix-Panabieres (1326_CR7) 2017; 63 Y Tang (1326_CR12) 2017; 114 S Ogino (1326_CR8) 2009; 27 Q Li (1326_CR17) 2017; 42 J He (1326_CR15) 2016; 9 K Pantel (1326_CR2) 2019; 16 DJ Smit (1326_CR10) 2020; 9 LE Cortés-Hernández (1326_CR4) 2020; 72 P Bu (1326_CR19) 2018; 27 N Weizman (1326_CR13) 2014; 33 C Alix-Panabières (1326_CR1) 2020; 579 L Cayrefourcq (1326_CR5) 2015; 75 QF Tao (1326_CR16) 2015; 14
References_xml	– volume: 8 start-page: 15931 issue: 1 year: 2018 ident: 1326_CR6 publication-title: Sci Rep doi: 10.1038/s41598-018-34365-z – volume: S1044-579X start-page: 30261 issue: 20 year: 2020 ident: 1326_CR11 publication-title: Semin Cancer Biol – volume: 12 start-page: e11908 issue: 9 year: 2020 ident: 1326_CR3 publication-title: EMBO Mol Med doi: 10.15252/emmm.201911908 – volume: 27 start-page: 1477 issue: 9 year: 2009 ident: 1326_CR8 publication-title: J Clin Oncol doi: 10.1200/JCO.2008.18.6544 – volume: 579 start-page: S9 issue: 7800 year: 2020 ident: 1326_CR1 publication-title: Nature. doi: 10.1038/d41586-020-00844-5 – volume: 114 start-page: 2544 issue: 10 year: 2017 ident: 1326_CR12 publication-title: Proc Natl Acad Sci doi: 10.1073/pnas.1612229114 – volume: 27 start-page: 1249 issue: 6 year: 2018 ident: 1326_CR19 publication-title: Cell Metab doi: 10.1016/j.cmet.2018.04.003 – volume: 16 start-page: 409 issue: 7 year: 2019 ident: 1326_CR2 publication-title: Nat Rev Clin Oncol doi: 10.1038/s41571-019-0187-3 – volume: 9 start-page: 6099 year: 2016 ident: 1326_CR15 publication-title: Onco Targets Ther doi: 10.2147/OTT.S110203 – volume: 42 start-page: 397 issue: 1 year: 2017 ident: 1326_CR17 publication-title: Cell Physiol Biochem doi: 10.1159/000477484 – volume: 63 start-page: 700 issue: 3 year: 2017 ident: 1326_CR7 publication-title: Clin Chem doi: 10.1373/clinchem.2016.263582 – volume: 19 start-page: 649 issue: 8 year: 2017 ident: 1326_CR14 publication-title: Neoplasia (New York, NY) doi: 10.1016/j.neo.2017.05.002 – volume: 33 start-page: 3812 issue: 29 year: 2014 ident: 1326_CR13 publication-title: Oncogene. doi: 10.1038/onc.2013.357 – volume: 14 start-page: 170 year: 2015 ident: 1326_CR16 publication-title: Mol Cancer doi: 10.1186/s12943-015-0437-7 – volume: 86 start-page: 38 issue: 1 year: 1993 ident: 1326_CR18 publication-title: South Med J doi: 10.1097/00007611-199301000-00009 – volume: 72 start-page: 100816 year: 2020 ident: 1326_CR4 publication-title: Mol Asp Med doi: 10.1016/j.mam.2019.07.008 – volume: 75 start-page: 892 issue: 5 year: 2015 ident: 1326_CR5 publication-title: Cancer Res doi: 10.1158/0008-5472.CAN-14-2613 – volume: 20 start-page: 1217 issue: 12 year: 2019 ident: 1326_CR9 publication-title: Curr Drug Targets doi: 10.2174/1389450120666190618123846 – volume: 9 start-page: 2129 issue: 9 year: 2020 ident: 1326_CR10 publication-title: Cells doi: 10.3390/cells9092129
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Snippet	The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator of... Abstract The characterization of circulating tumor cells (CTCs) holds promises for precision medicine because these cells are an important clinical indicator...
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SubjectTerms	1-Phosphatidylinositol 3-kinase 5-Fluorouracil AKT protein ALDOB Biochemistry, Molecular Biology Biomarkers Biomarkers, Tumor Biopsy Cancer Cancer therapies CDA Chemotherapy Circulating tumor cells Clonal evolution Cloning Colon cancer Colonic Neoplasms Colonic Neoplasms - genetics Colonic Neoplasms - pathology Colonic Neoplasms - therapy Colorectal cancer Computational Biology Computational Biology - methods Cytidine deaminase Detoxification Development and progression Drug resistance Drug Resistance, Neoplasm Drug Resistance, Neoplasm - drug effects Drug therapy Energy metabolism Enzymes Gene expression Gene Expression Profiling Genes Genomics Human health and pathology Humans Hépatology and Gastroenterology Letter to the Editor Life Sciences Liver Liver Neoplasms Liver Neoplasms - metabolism Liver Neoplasms - secondary Metabolism Metastases Metastasis Neoplasm Metastasis Neoplasm Staging Neoplastic Cells, Circulating Neoplastic Cells, Circulating - drug effects Neoplastic Cells, Circulating - metabolism Neoplastic Cells, Circulating - pathology Patients Peripheral blood Physiological aspects Precision medicine Stem cells TOR protein Transcriptome Tumor cells Tumors Xenobiotics
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Title	Selective treatment pressure in colon cancer drives the molecular profile of resistant circulating tumor cell clones
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