Literature DB >> 11672768

Comparative genomic hybridization analysis identifies gains of 1p35 approximately p36 and chromosome 19 in osteosarcoma.

M Zielenska1, J Bayani, A Pandita, S Toledo, P Marrano, J Andrade, A Petrilli, P Thorner, P Sorensen, J A Squire.   

Abstract

Osteosarcomas (OS) are aggressive tumors of the bone and often have a poor prognosis. Conventional cytogenetic analyses of OS have revealed highly complex karyotypes, with numerous abnormalities. In this study, we analyzed 18 untreated OS tumors from 17 patients of the younger incidence age group by comparative genomic hybridization (CGH), 4 tumors by spectral karyotyping (SKY) and fluorescence in situ hybridization (FISH). Comparative genomic hybridization identified frequent copy number changes of the chromosomal region 1p (10/17) and gain of part or all of chromosome 19(8/17). In addition gains were observed at 5p(3/17), 8q(3/17), 16p(3/17), and 17p(5/17); and losses at chromosomes 2q(3/17), 10(4/17) and 13(3/17). High level gains were detected in the 8q23 approximately q24 region in two tumors as well as at 17p in one primary and a metastatic tumor. Minimal regions of gain were present at 1p35 approximately p36.3 (8/17); 5p14 approximately p15.2 (3/17), and 8q22 approximately q24.3 (3/17). SKY analysis demonstrated that OS has a complex pattern of clonal and non-clonal rearrangements and helped confirm the structural basis for the imbalances detected by CGH. Spectral karyotyping confirmed an overall pattern of chromosomal gain affecting 1p in all four tumors. Fluorescence in situ hybridization analysis from these tumors confirmed the gain of the 1p36 region in 2 tumors as determined by CGH analysis as well as the amplification of 8q.

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Year:  2001        PMID: 11672768     DOI: 10.1016/s0165-4608(01)00461-7

Source DB:  PubMed          Journal:  Cancer Genet Cytogenet        ISSN: 0165-4608


  21 in total

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2.  Biomarkers in Osteosarcoma.

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Journal:  J Mol Diagn       Date:  2011-03-31       Impact factor: 5.568

4.  Evaluation of paediatric osteosarcomas by classic cytogenetic and CGH analyses.

Authors:  J R Batanian; L R Cavalli; N M Aldosari; E Ma; C Sotelo-Avila; M B Ramos; J D Rone; C M Thorpe; B R Haddad
Journal:  Mol Pathol       Date:  2002-12

5.  Distinct patterns of structural and numerical chromosomal instability characterize sporadic ovarian cancer.

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6.  Cell cycle regulator gene CDC5L, a potential target for 6p12-p21 amplicon in osteosarcoma.

Authors:  Xin-Yan Lu; Yaojuan Lu; Yi-Jue Zhao; Kim Jaeweon; Jason Kang; Li Xiao-Nan; Gouqing Ge; Rene Meyer; Laszlo Perlaky; John Hicks; Murali Chintagumpala; Wei-Wen Cai; Marc Ladanyi; Richard Gorlick; Ching C Lau; Debananda Pati; Michael Sheldon; Pulivarthi H Rao
Journal:  Mol Cancer Res       Date:  2008-06       Impact factor: 5.852

7.  Decitabine-induced demethylation of 5' CpG island in GADD45A leads to apoptosis in osteosarcoma cells.

Authors:  Khaldoun Al-Romaih; Bekim Sadikovic; Maisa Yoshimoto; Yuzhuo Wang; Maria Zielenska; Jeremy A Squire
Journal:  Neoplasia       Date:  2008-05       Impact factor: 5.715

8.  Recurrent RECQL4 imbalance and increased gene expression levels are associated with structural chromosomal instability in sporadic osteosarcoma.

Authors:  Georges Maire; Maisa Yoshimoto; Susan Chilton-MacNeill; Paul S Thorner; Maria Zielenska; Jeremy A Squire
Journal:  Neoplasia       Date:  2009-03       Impact factor: 5.715

9.  TRIO amplification and abundant mRNA expression is associated with invasive tumor growth and rapid tumor cell proliferation in urinary bladder cancer.

Authors:  Min Zheng; Ronald Simon; Martina Mirlacher; Robert Maurer; Thomas Gasser; Thomas Forster; Pierre Andre Diener; Michael J Mihatsch; Guido Sauter; Peter Schraml
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Review 10.  Osteosarcoma Genetics and Epigenetics: Emerging Biology and Candidate Therapies.

Authors:  James J Morrow; Chand Khanna
Journal:  Crit Rev Oncog       Date:  2015
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