Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts.

Ekkehard Dikomey; Kerstin Borgmann; Ingo Brammer; Ulla Kasten-Pisula

Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts.

Standard

Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts. / Dikomey, Ekkehard; Borgmann, Kerstin; Brammer, Ingo; Kasten-Pisula, Ulla.

in: TOXICOLOGY, Jahrgang 193, Nr. 1-2, 1-2, 2003, S. 125-135.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Dikomey, E, Borgmann, K, Brammer, I & Kasten-Pisula, U 2003, 'Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts.', TOXICOLOGY, Jg. 193, Nr. 1-2, 1-2, S. 125-135. <http://www.ncbi.nlm.nih.gov/pubmed/14599772?dopt=Citation>

APA

Dikomey, E., Borgmann, K., Brammer, I., & Kasten-Pisula, U. (2003). Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts. TOXICOLOGY, 193(1-2), 125-135. [1-2]. http://www.ncbi.nlm.nih.gov/pubmed/14599772?dopt=Citation

Vancouver

Dikomey E, Borgmann K, Brammer I, Kasten-Pisula U. Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts. TOXICOLOGY. 2003;193(1-2):125-135. 1-2.

Bibtex

@article{cdbc6a69cfae46d1aa301d6476594053,

title = "Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts.",

abstract = "The molecular mechanisms of individual radiosensitivity were studied in normal diploid human fibroblasts. For fibroblasts irradiated with X-rays in G1-phase the individual radiosensitivity was shown to be correlated with the extent of double-strand break (dsb) repair. The number of residual dsbs (including both non- and mis-rejoined dsbs) varied between 2 and 5% of the initial number induced and was low for resistant and high for sensitive strains. In the G1-phase dsbs are considered to be mostly repaired via the non-homologous end-joining pathway (NHEJ). However, so far none of the parameters tested for this pathway was found to be correlated with the number of residual dsbs. The parameters tested were mRNA expression, protein level and localisation and activity of the DNA-PK, which is the central complex of NHEJ. The dsb-repair capacity is also not regulated by the differentiation status, which varies substantially among fibroblast strains, whereas there is some indication that dsb repair might depend on the chromatin structure, with more efficient repair in cells with condensed DNA.Residual dsbs are converted into lethal chromosome aberrations finally leading to the loss of clonogenic activity, when cells pass through mitosis. Beside this so-called mitotic death, X-irradiated human fibroblasts are also inactivated via the TP53-dependent permanent G1-arrest, while apoptosis appears to be not important. On average, mitotic death and G1-arrest are equally effective, but there is a broad variation from one strain to the other, with a negative correlation between these two pathways. Fibroblast strains exhibiting only a moderate G1-arrest showed a high number of lethal aberrations and vice versa. This result points to a common regulator of both G1-arrest and dsb repair, which is presently under investigation.",

author = "Ekkehard Dikomey and Kerstin Borgmann and Ingo Brammer and Ulla Kasten-Pisula",

year = "2003",

language = "Deutsch",

volume = "193",

pages = "125--135",

journal = "TOXICOLOGY",

issn = "0300-483X",

publisher = "Elsevier Ireland Ltd",

number = "1-2",

}

RIS

TY - JOUR

T1 - Molecular mechanisms of individual radiosensitivity studied in normal diploid human fibroblasts.

AU - Dikomey, Ekkehard

AU - Borgmann, Kerstin

AU - Brammer, Ingo

AU - Kasten-Pisula, Ulla

PY - 2003

Y1 - 2003

N2 - The molecular mechanisms of individual radiosensitivity were studied in normal diploid human fibroblasts. For fibroblasts irradiated with X-rays in G1-phase the individual radiosensitivity was shown to be correlated with the extent of double-strand break (dsb) repair. The number of residual dsbs (including both non- and mis-rejoined dsbs) varied between 2 and 5% of the initial number induced and was low for resistant and high for sensitive strains. In the G1-phase dsbs are considered to be mostly repaired via the non-homologous end-joining pathway (NHEJ). However, so far none of the parameters tested for this pathway was found to be correlated with the number of residual dsbs. The parameters tested were mRNA expression, protein level and localisation and activity of the DNA-PK, which is the central complex of NHEJ. The dsb-repair capacity is also not regulated by the differentiation status, which varies substantially among fibroblast strains, whereas there is some indication that dsb repair might depend on the chromatin structure, with more efficient repair in cells with condensed DNA.Residual dsbs are converted into lethal chromosome aberrations finally leading to the loss of clonogenic activity, when cells pass through mitosis. Beside this so-called mitotic death, X-irradiated human fibroblasts are also inactivated via the TP53-dependent permanent G1-arrest, while apoptosis appears to be not important. On average, mitotic death and G1-arrest are equally effective, but there is a broad variation from one strain to the other, with a negative correlation between these two pathways. Fibroblast strains exhibiting only a moderate G1-arrest showed a high number of lethal aberrations and vice versa. This result points to a common regulator of both G1-arrest and dsb repair, which is presently under investigation.

AB - The molecular mechanisms of individual radiosensitivity were studied in normal diploid human fibroblasts. For fibroblasts irradiated with X-rays in G1-phase the individual radiosensitivity was shown to be correlated with the extent of double-strand break (dsb) repair. The number of residual dsbs (including both non- and mis-rejoined dsbs) varied between 2 and 5% of the initial number induced and was low for resistant and high for sensitive strains. In the G1-phase dsbs are considered to be mostly repaired via the non-homologous end-joining pathway (NHEJ). However, so far none of the parameters tested for this pathway was found to be correlated with the number of residual dsbs. The parameters tested were mRNA expression, protein level and localisation and activity of the DNA-PK, which is the central complex of NHEJ. The dsb-repair capacity is also not regulated by the differentiation status, which varies substantially among fibroblast strains, whereas there is some indication that dsb repair might depend on the chromatin structure, with more efficient repair in cells with condensed DNA.Residual dsbs are converted into lethal chromosome aberrations finally leading to the loss of clonogenic activity, when cells pass through mitosis. Beside this so-called mitotic death, X-irradiated human fibroblasts are also inactivated via the TP53-dependent permanent G1-arrest, while apoptosis appears to be not important. On average, mitotic death and G1-arrest are equally effective, but there is a broad variation from one strain to the other, with a negative correlation between these two pathways. Fibroblast strains exhibiting only a moderate G1-arrest showed a high number of lethal aberrations and vice versa. This result points to a common regulator of both G1-arrest and dsb repair, which is presently under investigation.

M3 - SCORING: Zeitschriftenaufsatz

VL - 193

SP - 125

EP - 135

JO - TOXICOLOGY

JF - TOXICOLOGY

SN - 0300-483X

IS - 1-2

M1 - 1-2

ER -