Integrated time course omics analysis distinguishes immediate therapeutic response from acquired resistance

Genevieve Stein-O'Brien; Luciane T. Kagohara; Sijia Li; Manjusha Thakar; Ruchira Ranaweera; Hiroyuki Ozawa; Haixia Cheng; Michael Considine; Sandra Schmitz; Alexander V. Favorov; Ludmila V. Danilova; Joseph A. Califano; Evgeny Izumchenko; Daria A. Gaykalova; Christine H. Chung; Elana J. Fertig

doi:10.1186/s13073-018-0545-2

Integrated time course omics analysis distinguishes immediate therapeutic response from acquired resistance

Genevieve Stein-O'Brien, Luciane T. Kagohara, Sijia Li, Manjusha Thakar, Ruchira Ranaweera, Hiroyuki Ozawa, Haixia Cheng, Michael Considine, Sandra Schmitz, Alexander V. Favorov, Ludmila V. Danilova, Joseph A. Califano, Evgeny Izumchenko, Daria A. Gaykalova, Christine H. Chung, Elana J. Fertig

School of Medicine

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

Abstract

Background: Targeted therapies specifically act by blocking the activity of proteins that are encoded by genes critical for tumorigenesis. However, most cancers acquire resistance and long-term disease remission is rarely observed. Understanding the time course of molecular changes responsible for the development of acquired resistance could enable optimization of patients' treatment options. Clinically, acquired therapeutic resistance can only be studied at a single time point in resistant tumors. Methods: To determine the dynamics of these molecular changes, we obtained high throughput omics data (RNA-sequencing and DNA methylation) weekly during the development of cetuximab resistance in a head and neck cancer in vitro model. The CoGAPS unsupervised algorithm was used to determine the dynamics of the molecular changes associated with resistance during the time course of resistance development. Results: CoGAPS was used to quantify the evolving transcriptional and epigenetic changes. Applying a PatternMarker statistic to the results from CoGAPS enabled novel heatmap-based visualization of the dynamics in these time course omics data. We demonstrate that transcriptional changes result from immediate therapeutic response or resistance, whereas epigenetic alterations only occur with resistance. Integrated analysis demonstrates delayed onset of changes in DNA methylation relative to transcription, suggesting that resistance is stabilized epigenetically. Conclusions: Genes with epigenetic alterations associated with resistance that have concordant expression changes are hypothesized to stabilize the resistant phenotype. These genes include FGFR1, which was associated with EGFR inhibitors resistance previously. Thus, integrated omics analysis distinguishes the timing of molecular drivers of resistance. This understanding of the time course progression of molecular changes in acquired resistance is important for the development of alternative treatment strategies that would introduce appropriate selection of new drugs to treat cancer before the resistant phenotype develops.

Original language	English (US)
Article number	37
Journal	Genome Medicine
Volume	10
Issue number	1
DOIs	https://doi.org/10.1186/s13073-018-0545-2
State	Published - May 23 2018

Keywords

Acquired resistance
Data integration
Epigenetics
Genomics
Precision medicine
Time course analysis

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Genetics
Genetics(clinical)

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10.1186/s13073-018-0545-2

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Stein-O'Brien, G., Kagohara, L. T., Li, S., Thakar, M., Ranaweera, R., Ozawa, H., Cheng, H., Considine, M., Schmitz, S., Favorov, A. V., Danilova, L. V., Califano, J. A., Izumchenko, E., Gaykalova, D. A., Chung, C. H., & Fertig, E. J. (2018). Integrated time course omics analysis distinguishes immediate therapeutic response from acquired resistance. Genome Medicine, 10(1), Article 37. https://doi.org/10.1186/s13073-018-0545-2

Stein-O'Brien, G , Kagohara, LT, Li, S, Thakar, M, Ranaweera, R, Ozawa, H, Cheng, H, Considine, M, Schmitz, S, Favorov, AV , Danilova, LV, Califano, JA, Izumchenko, E, Gaykalova, DA, Chung, CH & Fertig, EJ 2018, 'Integrated time course omics analysis distinguishes immediate therapeutic response from acquired resistance', Genome Medicine, vol. 10, no. 1, 37. https://doi.org/10.1186/s13073-018-0545-2

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title = "Integrated time course omics analysis distinguishes immediate therapeutic response from acquired resistance",

abstract = "Background: Targeted therapies specifically act by blocking the activity of proteins that are encoded by genes critical for tumorigenesis. However, most cancers acquire resistance and long-term disease remission is rarely observed. Understanding the time course of molecular changes responsible for the development of acquired resistance could enable optimization of patients' treatment options. Clinically, acquired therapeutic resistance can only be studied at a single time point in resistant tumors. Methods: To determine the dynamics of these molecular changes, we obtained high throughput omics data (RNA-sequencing and DNA methylation) weekly during the development of cetuximab resistance in a head and neck cancer in vitro model. The CoGAPS unsupervised algorithm was used to determine the dynamics of the molecular changes associated with resistance during the time course of resistance development. Results: CoGAPS was used to quantify the evolving transcriptional and epigenetic changes. Applying a PatternMarker statistic to the results from CoGAPS enabled novel heatmap-based visualization of the dynamics in these time course omics data. We demonstrate that transcriptional changes result from immediate therapeutic response or resistance, whereas epigenetic alterations only occur with resistance. Integrated analysis demonstrates delayed onset of changes in DNA methylation relative to transcription, suggesting that resistance is stabilized epigenetically. Conclusions: Genes with epigenetic alterations associated with resistance that have concordant expression changes are hypothesized to stabilize the resistant phenotype. These genes include FGFR1, which was associated with EGFR inhibitors resistance previously. Thus, integrated omics analysis distinguishes the timing of molecular drivers of resistance. This understanding of the time course progression of molecular changes in acquired resistance is important for the development of alternative treatment strategies that would introduce appropriate selection of new drugs to treat cancer before the resistant phenotype develops.",

keywords = "Acquired resistance, Data integration, Epigenetics, Genomics, Precision medicine, Time course analysis",

author = "Genevieve Stein-O'Brien and Kagohara, {Luciane T.} and Sijia Li and Manjusha Thakar and Ruchira Ranaweera and Hiroyuki Ozawa and Haixia Cheng and Michael Considine and Sandra Schmitz and Favorov, {Alexander V.} and Danilova, {Ludmila V.} and Califano, {Joseph A.} and Evgeny Izumchenko and Gaykalova, {Daria A.} and Chung, {Christine H.} and Fertig, {Elana J.}",

note = "Publisher Copyright: {\textcopyright} 2018 The Author(s).",

year = "2018",

month = may,

day = "23",

doi = "10.1186/s13073-018-0545-2",

language = "English (US)",

volume = "10",

journal = "Genome Medicine",

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T1 - Integrated time course omics analysis distinguishes immediate therapeutic response from acquired resistance

AU - Stein-O'Brien, Genevieve

AU - Kagohara, Luciane T.

AU - Li, Sijia

AU - Thakar, Manjusha

AU - Ranaweera, Ruchira

AU - Ozawa, Hiroyuki

AU - Cheng, Haixia

AU - Considine, Michael

AU - Schmitz, Sandra

AU - Favorov, Alexander V.

AU - Danilova, Ludmila V.

AU - Califano, Joseph A.

AU - Izumchenko, Evgeny

AU - Gaykalova, Daria A.

AU - Chung, Christine H.

AU - Fertig, Elana J.

PY - 2018/5/23

Y1 - 2018/5/23

N2 - Background: Targeted therapies specifically act by blocking the activity of proteins that are encoded by genes critical for tumorigenesis. However, most cancers acquire resistance and long-term disease remission is rarely observed. Understanding the time course of molecular changes responsible for the development of acquired resistance could enable optimization of patients' treatment options. Clinically, acquired therapeutic resistance can only be studied at a single time point in resistant tumors. Methods: To determine the dynamics of these molecular changes, we obtained high throughput omics data (RNA-sequencing and DNA methylation) weekly during the development of cetuximab resistance in a head and neck cancer in vitro model. The CoGAPS unsupervised algorithm was used to determine the dynamics of the molecular changes associated with resistance during the time course of resistance development. Results: CoGAPS was used to quantify the evolving transcriptional and epigenetic changes. Applying a PatternMarker statistic to the results from CoGAPS enabled novel heatmap-based visualization of the dynamics in these time course omics data. We demonstrate that transcriptional changes result from immediate therapeutic response or resistance, whereas epigenetic alterations only occur with resistance. Integrated analysis demonstrates delayed onset of changes in DNA methylation relative to transcription, suggesting that resistance is stabilized epigenetically. Conclusions: Genes with epigenetic alterations associated with resistance that have concordant expression changes are hypothesized to stabilize the resistant phenotype. These genes include FGFR1, which was associated with EGFR inhibitors resistance previously. Thus, integrated omics analysis distinguishes the timing of molecular drivers of resistance. This understanding of the time course progression of molecular changes in acquired resistance is important for the development of alternative treatment strategies that would introduce appropriate selection of new drugs to treat cancer before the resistant phenotype develops.

AB - Background: Targeted therapies specifically act by blocking the activity of proteins that are encoded by genes critical for tumorigenesis. However, most cancers acquire resistance and long-term disease remission is rarely observed. Understanding the time course of molecular changes responsible for the development of acquired resistance could enable optimization of patients' treatment options. Clinically, acquired therapeutic resistance can only be studied at a single time point in resistant tumors. Methods: To determine the dynamics of these molecular changes, we obtained high throughput omics data (RNA-sequencing and DNA methylation) weekly during the development of cetuximab resistance in a head and neck cancer in vitro model. The CoGAPS unsupervised algorithm was used to determine the dynamics of the molecular changes associated with resistance during the time course of resistance development. Results: CoGAPS was used to quantify the evolving transcriptional and epigenetic changes. Applying a PatternMarker statistic to the results from CoGAPS enabled novel heatmap-based visualization of the dynamics in these time course omics data. We demonstrate that transcriptional changes result from immediate therapeutic response or resistance, whereas epigenetic alterations only occur with resistance. Integrated analysis demonstrates delayed onset of changes in DNA methylation relative to transcription, suggesting that resistance is stabilized epigenetically. Conclusions: Genes with epigenetic alterations associated with resistance that have concordant expression changes are hypothesized to stabilize the resistant phenotype. These genes include FGFR1, which was associated with EGFR inhibitors resistance previously. Thus, integrated omics analysis distinguishes the timing of molecular drivers of resistance. This understanding of the time course progression of molecular changes in acquired resistance is important for the development of alternative treatment strategies that would introduce appropriate selection of new drugs to treat cancer before the resistant phenotype develops.

KW - Acquired resistance

KW - Data integration

KW - Epigenetics

KW - Genomics

KW - Precision medicine

KW - Time course analysis

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Integrated time course omics analysis distinguishes immediate therapeutic response from acquired resistance

Abstract

Keywords

ASJC Scopus subject areas

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