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Comparative genomic hybridization detects many recurrent imbalances in central nervous system primitive neuroectodermal tumours in children
Authors
A Lellouch-Tubiana
A-M Vénuat
+33 more
AM Vagner-Capodano
BR Schutz
CA Griffin
DA Reardon
DF Callen
E Neumann
E Rouah
FG Barker
G Vassal
GN Fuller
H Avet-Loiseau
J Jen
J McDonald
JA Biegel
JA Biegel
JA Biegel
JC Wasson
JR Farwell
M Badiali
M Meddeb
M Paszek-Vigier
M Wolter
M Zerah
M-J Terrier-Lacombe
OP Kallioniemi
PH Cogen
PS Karnes
S Batra
SH Bigner
SH Bigner
T Pietsch
WG Scheurlen
Y Fujii
Publication date
Publisher
Nature Publishing Group
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on
PubMed
Abstract
A series of 23 children with primitive neuroectodermal tumours (PNET) were analysed with comparative genomic hybridization (CGH). Multiple chromosomal imbalances have been detected in 20 patients. The most frequently involved chromosome was chromosome 17, with a gain of 17q (11 cases) and loss of 17p (eight cases). Further recurrent copy number changes were detected. Extra copies of chromosome 7 were present in nine patients and gains of 1q were detected in six patients. A moderate genomic amplification was detected in one patient, involving two sites on 3p and the whole 12p. Losses were more frequent, and especially involved the chromosomes 11 (nine cases), 10q (eight cases), 8 (six cases), X (six patients) and 3 (five cases), and part of chromosome 9 (five cases). These recurrent chromosomal changes may highlight locations of novel genes with an important role in the development and/or progression of PNET. © 1999 Cancer Research Campaig
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Last time updated on 03/01/2020