Chromosomal breakage-fusion-bridge events cause genetic intratumor heterogeneity

Gisselsson Nord, David; Pettersson, Louise; Höglund, Mattias; Heidenblad, Markus; Gorunova, Ludmila; Wiegant, J; Mertens, Fredrik; Dal Cin, P; Mitelman, Felix; Mandahl, Nils

Chromosomal breakage-fusion-bridge events cause genetic intratumor heterogeneity

Mark

Gisselsson Nord, David ^LU ; Pettersson, Louise ; Höglund, Mattias ^LU ; Heidenblad, Markus ^LU ; Gorunova, Ludmila ^LU ; Wiegant, J ; Mertens, Fredrik ^LU ; Dal Cin, P ; Mitelman, Felix ^LU

and Mandahl, Nils ^LU (2000) In Proceedings of the National Academy of Sciences 97(10). p.5357-5362

Abstract: It has long been known that rearrangements of chromosomes through breakage-fusion-bridge (BFB) cycles may cause variability of phenotypic and genetic traits within a cell population. Because intercellular heterogeneity is often found in neoplastic tissues, we investigated the occurrence of BFB events in human solid tumors. Evidence of frequent BFB events was found in malignancies that showed unspecific chromosome aberrations, including ring chromosomes, dicentric chromosomes, and telomeric associations, as well as extensive intratumor heterogeneity in the pattern of structural changes but not in tumors with tumor-specific aberrations and low variability. Fluorescence in situ hybridization analysis demonstrated that chromosomes... (More); It has long been known that rearrangements of chromosomes through breakage-fusion-bridge (BFB) cycles may cause variability of phenotypic and genetic traits within a cell population. Because intercellular heterogeneity is often found in neoplastic tissues, we investigated the occurrence of BFB events in human solid tumors. Evidence of frequent BFB events was found in malignancies that showed unspecific chromosome aberrations, including ring chromosomes, dicentric chromosomes, and telomeric associations, as well as extensive intratumor heterogeneity in the pattern of structural changes but not in tumors with tumor-specific aberrations and low variability. Fluorescence in situ hybridization analysis demonstrated that chromosomes participating in anaphase bridge formation were involved in a significantly higher number of structural aberrations than other chromosomes. Tumors with BFB events showed a decreased elimination rate of unstable chromosome aberrations after irradiation compared with normal cells and other tumor cells. This result suggests that a combination of mitotically unstable chromosomes and an elevated tolerance to chromosomal damage leads to constant genomic reorganization in many malignancies, thereby providing a flexible genetic system for clonal evolution and progression. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1116706

author

Gisselsson Nord, David ^LU ; Pettersson, Louise ; Höglund, Mattias ^LU ; Heidenblad, Markus ^LU ; Gorunova, Ludmila ^LU ; Wiegant, J ; Mertens, Fredrik ^LU ; Dal Cin, P ; Mitelman, Felix ^LU

and Mandahl, Nils ^LU

organization

publishing date

2000

type

Contribution to journal

publication status

published

subject

Medical Genetics

in

Proceedings of the National Academy of Sciences

volume

97

issue

10

pages

5357 - 5362

publisher

National Academy of Sciences

external identifiers

pmid:10805796
scopus:12944329959
pmid:10805796

ISSN

1091-6490

DOI

10.1073/pnas.090013497

language

English

LU publication?

yes

id

8e764f78-bc02-4f8a-84fb-068ece20c611 (old id 1116706)

date added to LUP

2016-04-01 11:36:31

date last changed

2022-06-01 20:44:27

@article{8e764f78-bc02-4f8a-84fb-068ece20c611,
  abstract     = {{It has long been known that rearrangements of chromosomes through breakage-fusion-bridge (BFB) cycles may cause variability of phenotypic and genetic traits within a cell population. Because intercellular heterogeneity is often found in neoplastic tissues, we investigated the occurrence of BFB events in human solid tumors. Evidence of frequent BFB events was found in malignancies that showed unspecific chromosome aberrations, including ring chromosomes, dicentric chromosomes, and telomeric associations, as well as extensive intratumor heterogeneity in the pattern of structural changes but not in tumors with tumor-specific aberrations and low variability. Fluorescence in situ hybridization analysis demonstrated that chromosomes participating in anaphase bridge formation were involved in a significantly higher number of structural aberrations than other chromosomes. Tumors with BFB events showed a decreased elimination rate of unstable chromosome aberrations after irradiation compared with normal cells and other tumor cells. This result suggests that a combination of mitotically unstable chromosomes and an elevated tolerance to chromosomal damage leads to constant genomic reorganization in many malignancies, thereby providing a flexible genetic system for clonal evolution and progression.}},
  author       = {{Gisselsson Nord, David and Pettersson, Louise and Höglund, Mattias and Heidenblad, Markus and Gorunova, Ludmila and Wiegant, J and Mertens, Fredrik and Dal Cin, P and Mitelman, Felix and Mandahl, Nils}},
  issn         = {{1091-6490}},
  language     = {{eng}},
  number       = {{10}},
  pages        = {{5357--5362}},
  publisher    = {{National Academy of Sciences}},
  series       = {{Proceedings of the National Academy of Sciences}},
  title        = {{Chromosomal breakage-fusion-bridge events cause genetic intratumor heterogeneity}},
  url          = {{http://dx.doi.org/10.1073/pnas.090013497}},
  doi          = {{10.1073/pnas.090013497}},
  volume       = {{97}},
  year         = {{2000}},
}

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Chromosomal breakage-fusion-bridge events cause genetic intratumor heterogeneity