Genetic and transcriptional evolution alters cancer cell line drug response

Uri Ben-David; Benjamin Siranosian; Gavin Ha; Helen Tang; Yaara Oren; Kunihiko Hinohara; Craig A. Strathdee; Joshua Dempster; Nicholas J. Lyons; Robert Burns; Anwesha Nag; Guillaume Kugener; Beth Cimini; Peter Tsvetkov; Yosef E. Maruvka; Ryan O’Rourke; Anthony Garrity; Andrew A. Tubelli; Pratiti Bandopadhayay; Aviad Tsherniak; Francisca Vazquez; Bang Wong; Chet Birger; Mahmoud Ghandi; Aaron R. Thorner; Joshua A. Bittker; Matthew Meyerson; Gad Getz; Rameen Beroukhim; Todd R. Golub

doi:https://doi.org/10.1038/s41586-018-0409-3

Genetic and transcriptional evolution alters cancer cell line drug response

Uri Ben-David, Benjamin Siranosian, Gavin Ha, Helen Tang, Yaara Oren, Kunihiko Hinohara, Craig A. Strathdee, Joshua Dempster, Nicholas J. Lyons, Robert Burns, Anwesha Nag, Guillaume Kugener, Beth Cimini, Peter Tsvetkov, Yosef E. Maruvka, Ryan O’Rourke, Anthony Garrity, Andrew A. Tubelli, Pratiti Bandopadhayay, Aviad TsherniakFrancisca Vazquez, Bang Wong, Chet Birger, Mahmoud Ghandi, Aaron R. Thorner, Joshua A. Bittker, Matthew Meyerson, Gad Getz, Rameen Beroukhim, Todd R. Golub

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

Abstract

Human cancer cell lines are the workhorse of cancer research. Although cell lines are known to evolve in culture, the extent of the resultant genetic and transcriptional heterogeneity and its functional consequences remain understudied. Here we use genomic analyses of 106 human cell lines grown in two laboratories to show extensive clonal diversity. Further comprehensive genomic characterization of 27 strains of the common breast cancer cell line MCF7 uncovered rapid genetic diversification. Similar results were obtained with multiple strains of 13 additional cell lines. Notably, genetic changes were associated with differential activation of gene expression programs and marked differences in cell morphology and proliferation. Barcoding experiments showed that cell line evolution occurs as a result of positive clonal selection that is highly sensitive to culture conditions. Analyses of single-cell-derived clones demonstrated that continuous instability quickly translates into heterogeneity of the cell line. When the 27 MCF7 strains were tested against 321 anti-cancer compounds, we uncovered considerably different drug responses: at least 75% of compounds that strongly inhibited some strains were completely inactive in others. This study documents the extent, origins and consequences of genetic variation within cell lines, and provides a framework for researchers to measure such variation in efforts to support maximally reproducible cancer research.

Original language	English
Pages (from-to)	325-330
Number of pages	6
Journal	Nature
Volume	560
Issue number	7718
DOIs	https://doi.org/10.1038/s41586-018-0409-3
State	Published - 16 Aug 2018
Externally published	Yes

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Ben-David, U., Siranosian, B., Ha, G., Tang, H., Oren, Y., Hinohara, K., Strathdee, C. A., Dempster, J., Lyons, N. J., Burns, R., Nag, A., Kugener, G., Cimini, B., Tsvetkov, P., Maruvka, Y. E., O’Rourke, R., Garrity, A., Tubelli, A. A., Bandopadhayay, P., ... Golub, T. R. (2018). Genetic and transcriptional evolution alters cancer cell line drug response. Nature, 560(7718), 325-330. https://doi.org/10.1038/s41586-018-0409-3

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title = "Genetic and transcriptional evolution alters cancer cell line drug response",

abstract = "Human cancer cell lines are the workhorse of cancer research. Although cell lines are known to evolve in culture, the extent of the resultant genetic and transcriptional heterogeneity and its functional consequences remain understudied. Here we use genomic analyses of 106 human cell lines grown in two laboratories to show extensive clonal diversity. Further comprehensive genomic characterization of 27 strains of the common breast cancer cell line MCF7 uncovered rapid genetic diversification. Similar results were obtained with multiple strains of 13 additional cell lines. Notably, genetic changes were associated with differential activation of gene expression programs and marked differences in cell morphology and proliferation. Barcoding experiments showed that cell line evolution occurs as a result of positive clonal selection that is highly sensitive to culture conditions. Analyses of single-cell-derived clones demonstrated that continuous instability quickly translates into heterogeneity of the cell line. When the 27 MCF7 strains were tested against 321 anti-cancer compounds, we uncovered considerably different drug responses: at least 75% of compounds that strongly inhibited some strains were completely inactive in others. This study documents the extent, origins and consequences of genetic variation within cell lines, and provides a framework for researchers to measure such variation in efforts to support maximally reproducible cancer research.",

author = "Uri Ben-David and Benjamin Siranosian and Gavin Ha and Helen Tang and Yaara Oren and Kunihiko Hinohara and Strathdee, {Craig A.} and Joshua Dempster and Lyons, {Nicholas J.} and Robert Burns and Anwesha Nag and Guillaume Kugener and Beth Cimini and Peter Tsvetkov and Maruvka, {Yosef E.} and Ryan O{\textquoteright}Rourke and Anthony Garrity and Tubelli, {Andrew A.} and Pratiti Bandopadhayay and Aviad Tsherniak and Francisca Vazquez and Bang Wong and Chet Birger and Mahmoud Ghandi and Thorner, {Aaron R.} and Bittker, {Joshua A.} and Matthew Meyerson and Gad Getz and Rameen Beroukhim and Golub, {Todd R.}",

note = "Publisher Copyright: {\textcopyright} 2018, Springer Nature Limited.",

year = "2018",

month = aug,

day = "16",

doi = "https://doi.org/10.1038/s41586-018-0409-3",

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Ben-David, U, Siranosian, B, Ha, G, Tang, H, Oren, Y, Hinohara, K, Strathdee, CA, Dempster, J, Lyons, NJ, Burns, R, Nag, A, Kugener, G, Cimini, B, Tsvetkov, P, Maruvka, YE, O’Rourke, R, Garrity, A, Tubelli, AA, Bandopadhayay, P, Tsherniak, A, Vazquez, F, Wong, B, Birger, C, Ghandi, M, Thorner, AR, Bittker, JA, Meyerson, M, Getz, G, Beroukhim, R & Golub, TR 2018, 'Genetic and transcriptional evolution alters cancer cell line drug response', Nature, vol. 560, no. 7718, pp. 325-330. https://doi.org/10.1038/s41586-018-0409-3

TY - JOUR

T1 - Genetic and transcriptional evolution alters cancer cell line drug response

AU - Ben-David, Uri

AU - Siranosian, Benjamin

AU - Ha, Gavin

AU - Tang, Helen

AU - Oren, Yaara

AU - Hinohara, Kunihiko

AU - Strathdee, Craig A.

AU - Dempster, Joshua

AU - Lyons, Nicholas J.

AU - Burns, Robert

AU - Nag, Anwesha

AU - Kugener, Guillaume

AU - Cimini, Beth

AU - Tsvetkov, Peter

AU - Maruvka, Yosef E.

AU - O’Rourke, Ryan

AU - Garrity, Anthony

AU - Tubelli, Andrew A.

AU - Bandopadhayay, Pratiti

AU - Tsherniak, Aviad

AU - Vazquez, Francisca

AU - Wong, Bang

AU - Birger, Chet

AU - Ghandi, Mahmoud

AU - Thorner, Aaron R.

AU - Bittker, Joshua A.

AU - Meyerson, Matthew

AU - Getz, Gad

AU - Beroukhim, Rameen

AU - Golub, Todd R.

PY - 2018/8/16

Y1 - 2018/8/16

N2 - Human cancer cell lines are the workhorse of cancer research. Although cell lines are known to evolve in culture, the extent of the resultant genetic and transcriptional heterogeneity and its functional consequences remain understudied. Here we use genomic analyses of 106 human cell lines grown in two laboratories to show extensive clonal diversity. Further comprehensive genomic characterization of 27 strains of the common breast cancer cell line MCF7 uncovered rapid genetic diversification. Similar results were obtained with multiple strains of 13 additional cell lines. Notably, genetic changes were associated with differential activation of gene expression programs and marked differences in cell morphology and proliferation. Barcoding experiments showed that cell line evolution occurs as a result of positive clonal selection that is highly sensitive to culture conditions. Analyses of single-cell-derived clones demonstrated that continuous instability quickly translates into heterogeneity of the cell line. When the 27 MCF7 strains were tested against 321 anti-cancer compounds, we uncovered considerably different drug responses: at least 75% of compounds that strongly inhibited some strains were completely inactive in others. This study documents the extent, origins and consequences of genetic variation within cell lines, and provides a framework for researchers to measure such variation in efforts to support maximally reproducible cancer research.

AB - Human cancer cell lines are the workhorse of cancer research. Although cell lines are known to evolve in culture, the extent of the resultant genetic and transcriptional heterogeneity and its functional consequences remain understudied. Here we use genomic analyses of 106 human cell lines grown in two laboratories to show extensive clonal diversity. Further comprehensive genomic characterization of 27 strains of the common breast cancer cell line MCF7 uncovered rapid genetic diversification. Similar results were obtained with multiple strains of 13 additional cell lines. Notably, genetic changes were associated with differential activation of gene expression programs and marked differences in cell morphology and proliferation. Barcoding experiments showed that cell line evolution occurs as a result of positive clonal selection that is highly sensitive to culture conditions. Analyses of single-cell-derived clones demonstrated that continuous instability quickly translates into heterogeneity of the cell line. When the 27 MCF7 strains were tested against 321 anti-cancer compounds, we uncovered considerably different drug responses: at least 75% of compounds that strongly inhibited some strains were completely inactive in others. This study documents the extent, origins and consequences of genetic variation within cell lines, and provides a framework for researchers to measure such variation in efforts to support maximally reproducible cancer research.

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U2 - https://doi.org/10.1038/s41586-018-0409-3

DO - https://doi.org/10.1038/s41586-018-0409-3

M3 - مقالة

C2 - 30089904

SN - 0028-0836

VL - 560

SP - 325

EP - 330

JO - Nature

JF - Nature

IS - 7718

ER -

Genetic and transcriptional evolution alters cancer cell line drug response

Abstract

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