Numerical chromosomal instability mediates susceptibility to radiation treatment

Samuel F. Bakhoum; Lilian Kabeche; Matthew D. Wood; Christopher D. Laucius; Dian Qu; Ashley M. Laughney; Gloria E. Reynolds; Raymond J. Louie; Joanna Phillips; Denise A. Chan; Bassem I. Zaki; John P. Murnane; Claudia Petritsch; Duane A. Compton

doi:10.1038/ncomms6990

Numerical chromosomal instability mediates susceptibility to radiation treatment

Samuel F. Bakhoum, Lilian Kabeche, Matthew D. Wood, Christopher D. Laucius, Dian Qu, Ashley M. Laughney, Gloria E. Reynolds, Raymond J. Louie, Joanna Phillips, Denise A. Chan, Bassem I. Zaki, John P. Murnane, Claudia Petritsch, Duane A. Compton

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

56 Scopus citations

Abstract

The exquisite sensitivity of mitotic cancer cells to ionizing radiation (IR) underlies an important rationale for the widely used fractionated radiation therapy. However, the mechanism for this cell cycle-dependent vulnerability is unknown. Here we show that treatment with IR leads to mitotic chromosome segregation errors in vivo and long-lasting aneuploidy in tumour-derived cell lines. These mitotic errors generate an abundance of micronuclei that predispose chromosomes to subsequent catastrophic pulverization thereby independently amplifying radiation-induced genome damage. Experimentally suppressing whole-chromosome missegregation reduces downstream chromosomal defects and significantly increases the viability of irradiated mitotic cells. Further, orthotopically transplanted human glioblastoma tumours in which chromosome missegregation rates have been reduced are rendered markedly more resistant to IR, exhibiting diminished markers of cell death in response to treatment. This work identifies a novel mitotic pathway for radiation-induced genome damage, which occurs outside of the primary nucleus and augments chromosomal breaks. This relationship between radiation treatment and whole-chromosome missegregation can be exploited to modulate therapeutic response in a clinically relevant manner.

Original language	English (US)
Article number	5990
Journal	Nature communications
Volume	6
DOIs	https://doi.org/10.1038/ncomms6990
State	Published - Jan 21 2015
Externally published	Yes

ASJC Scopus subject areas

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General Physics and Astronomy

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10.1038/ncomms6990

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@article{c6a737cfb73f4aeaa9dd98c0773f0722,

title = "Numerical chromosomal instability mediates susceptibility to radiation treatment",

abstract = "The exquisite sensitivity of mitotic cancer cells to ionizing radiation (IR) underlies an important rationale for the widely used fractionated radiation therapy. However, the mechanism for this cell cycle-dependent vulnerability is unknown. Here we show that treatment with IR leads to mitotic chromosome segregation errors in vivo and long-lasting aneuploidy in tumour-derived cell lines. These mitotic errors generate an abundance of micronuclei that predispose chromosomes to subsequent catastrophic pulverization thereby independently amplifying radiation-induced genome damage. Experimentally suppressing whole-chromosome missegregation reduces downstream chromosomal defects and significantly increases the viability of irradiated mitotic cells. Further, orthotopically transplanted human glioblastoma tumours in which chromosome missegregation rates have been reduced are rendered markedly more resistant to IR, exhibiting diminished markers of cell death in response to treatment. This work identifies a novel mitotic pathway for radiation-induced genome damage, which occurs outside of the primary nucleus and augments chromosomal breaks. This relationship between radiation treatment and whole-chromosome missegregation can be exploited to modulate therapeutic response in a clinically relevant manner.",

author = "Bakhoum, {Samuel F.} and Lilian Kabeche and Wood, {Matthew D.} and Laucius, {Christopher D.} and Dian Qu and Laughney, {Ashley M.} and Reynolds, {Gloria E.} and Louie, {Raymond J.} and Joanna Phillips and Chan, {Denise A.} and Zaki, {Bassem I.} and Murnane, {John P.} and Claudia Petritsch and Compton, {Duane A.}",

note = "Funding Information: We thank Bernardo Orr, Alan C. Hartford, Ethan Dmitrosvky and Hal Swartz (Dartmouth College), Mathieu Bakhoum (University of Texas Medical Branch), Giulio Genovese (Broad Institute of Harvard and MIT), Jeffrey Guenette (Harvard Medical School), Daphne Haas-Kogan (University of California San Francisco), Barry Rosenstein (Mount Sinai School of Medicine) and members of the Murnane (UCSF) and Compton (Dartmouth) Laboratories for critical feedback. This study was supported by the following grants: R37GM051542 (D.A. Compton), R01GM008704 (L.K.), R01CA120205 (J.P.M., G.E.R.) R01CA164746 and R01NS080619 (C.P., D.Q.) from the National Institutes of Health, and the John H. Copenhaver Jr and William H. Thomas, MD 1952 Junior Fellowship (L.K.), Hitchcock-Foundation 250-4041 and RSNA 1304 (S.B.).",

year = "2015",

month = jan,

day = "21",

doi = "10.1038/ncomms6990",

language = "English (US)",

volume = "6",

journal = "Nature communications",

issn = "2041-1723",

publisher = "Nature Publishing Group",

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TY - JOUR

T1 - Numerical chromosomal instability mediates susceptibility to radiation treatment

AU - Bakhoum, Samuel F.

AU - Kabeche, Lilian

AU - Wood, Matthew D.

AU - Laucius, Christopher D.

AU - Qu, Dian

AU - Laughney, Ashley M.

AU - Reynolds, Gloria E.

AU - Louie, Raymond J.

AU - Phillips, Joanna

AU - Chan, Denise A.

AU - Zaki, Bassem I.

AU - Murnane, John P.

AU - Petritsch, Claudia

AU - Compton, Duane A.

N1 - Funding Information: We thank Bernardo Orr, Alan C. Hartford, Ethan Dmitrosvky and Hal Swartz (Dartmouth College), Mathieu Bakhoum (University of Texas Medical Branch), Giulio Genovese (Broad Institute of Harvard and MIT), Jeffrey Guenette (Harvard Medical School), Daphne Haas-Kogan (University of California San Francisco), Barry Rosenstein (Mount Sinai School of Medicine) and members of the Murnane (UCSF) and Compton (Dartmouth) Laboratories for critical feedback. This study was supported by the following grants: R37GM051542 (D.A. Compton), R01GM008704 (L.K.), R01CA120205 (J.P.M., G.E.R.) R01CA164746 and R01NS080619 (C.P., D.Q.) from the National Institutes of Health, and the John H. Copenhaver Jr and William H. Thomas, MD 1952 Junior Fellowship (L.K.), Hitchcock-Foundation 250-4041 and RSNA 1304 (S.B.).

PY - 2015/1/21

Y1 - 2015/1/21

N2 - The exquisite sensitivity of mitotic cancer cells to ionizing radiation (IR) underlies an important rationale for the widely used fractionated radiation therapy. However, the mechanism for this cell cycle-dependent vulnerability is unknown. Here we show that treatment with IR leads to mitotic chromosome segregation errors in vivo and long-lasting aneuploidy in tumour-derived cell lines. These mitotic errors generate an abundance of micronuclei that predispose chromosomes to subsequent catastrophic pulverization thereby independently amplifying radiation-induced genome damage. Experimentally suppressing whole-chromosome missegregation reduces downstream chromosomal defects and significantly increases the viability of irradiated mitotic cells. Further, orthotopically transplanted human glioblastoma tumours in which chromosome missegregation rates have been reduced are rendered markedly more resistant to IR, exhibiting diminished markers of cell death in response to treatment. This work identifies a novel mitotic pathway for radiation-induced genome damage, which occurs outside of the primary nucleus and augments chromosomal breaks. This relationship between radiation treatment and whole-chromosome missegregation can be exploited to modulate therapeutic response in a clinically relevant manner.

AB - The exquisite sensitivity of mitotic cancer cells to ionizing radiation (IR) underlies an important rationale for the widely used fractionated radiation therapy. However, the mechanism for this cell cycle-dependent vulnerability is unknown. Here we show that treatment with IR leads to mitotic chromosome segregation errors in vivo and long-lasting aneuploidy in tumour-derived cell lines. These mitotic errors generate an abundance of micronuclei that predispose chromosomes to subsequent catastrophic pulverization thereby independently amplifying radiation-induced genome damage. Experimentally suppressing whole-chromosome missegregation reduces downstream chromosomal defects and significantly increases the viability of irradiated mitotic cells. Further, orthotopically transplanted human glioblastoma tumours in which chromosome missegregation rates have been reduced are rendered markedly more resistant to IR, exhibiting diminished markers of cell death in response to treatment. This work identifies a novel mitotic pathway for radiation-induced genome damage, which occurs outside of the primary nucleus and augments chromosomal breaks. This relationship between radiation treatment and whole-chromosome missegregation can be exploited to modulate therapeutic response in a clinically relevant manner.

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DO - 10.1038/ncomms6990

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SN - 2041-1723

VL - 6

JO - Nature communications

JF - Nature communications

M1 - 5990

ER -

Numerical chromosomal instability mediates susceptibility to radiation treatment

Abstract

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