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  5. Spontaneous and Radiation-Induced Chromosome Aberrations in Primary Fibroblasts of Patients With Pediatric First and Second Neoplasms
 
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2020
Zweitveröffentlichung
Artikel
Verlagsversion

Spontaneous and Radiation-Induced Chromosome Aberrations in Primary Fibroblasts of Patients With Pediatric First and Second Neoplasms

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Hauptpublikation
fonc-10-01338.pdf
CC BY 4.0 International
Format: Adobe PDF
Size: 1.61 MB
TUDa URI
tuda/7146
URN
urn:nbn:de:tuda-tuprints-189369
DOI
10.26083/tuprints-00018936
Autor:innen
Zahnreich, Sebastian
Poplawski, Alicia
Hartel, Carola
Eckhard, Lukas Stefan
Galetzka, Danuta
Hankeln, Thomas
Löbrich, Markus ORCID 0000-0003-3035-4048
Marron, Manuela
Mirsch, Johanna
Ritter, Sylvia
Scholz-Kreisel, Peter
Spix, Claudia
Schmidberger, Heinz
Kurzbeschreibung (Abstract)

The purpose of the present study was to investigate whether former childhood cancer patients who developed a subsequent secondary primary neoplasm (SPN) are characterized by elevated spontaneous chromosomal instability or cellular and chromosomal radiation sensitivity as surrogate markers of compromised DNA repair compared to childhood cancer patients with a first primary neoplasm (FPN) only or tumor-free controls. Primary skin fibroblasts were obtained in a nested case-control study including 23 patients with a pediatric FPN, 22 matched patients with a pediatric FPN and an SPN, and 22 matched tumor-free donors. Clonogenic cell survival and cytogenetic aberrations in Giemsa-stained first metaphases were assessed after X-irradiation in G1 or on prematurely condensed chromosomes of cells irradiated and analyzed in G2. Fluorescence in situ hybridization was applied to investigate spontaneous transmissible aberrations in selected donors. No significant difference in clonogenic survival or the average yield of spontaneous or radiation-induced aberrations was found between the study populations. However, two donors with an SPN showed striking spontaneous chromosomal instability occurring as high rates of numerical and structural aberrations or non-clonal and clonal translocations. No correlation was found between radiation sensitivity and a susceptibility to a pediatric FPN or a treatment-associated SPN. Together, the results of this unique case-control study show genomic stability and normal radiation sensitivity in normal somatic cells of donors with an early and high intrinsic or therapy-associated tumor risk. These findings provide valuable information for future studies on the etiology of sporadic childhood cancer and therapy-related SPN as well as for the establishment of predictive biomarkers based on altered DNA repair processes.

Sprache
Englisch
Fachbereich/-gebiet
10 Fachbereich Biologie > Radiation Biology and DNA Repair
DDC
500 Naturwissenschaften und Mathematik > 570 Biowissenschaften, Biologie
Institution
Universitäts- und Landesbibliothek Darmstadt
Ort
Darmstadt
Titel der Zeitschrift / Schriftenreihe
Frontiers in Oncology
Jahrgang der Zeitschrift
10
ISSN
2234-943X
Verlag
Frontiers
Publikationsjahr der Erstveröffentlichung
2020
Verlags-DOI
10.3389/fonc.2020.01338
PPN
510110363

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