Scholtysik, Rene and Kreuz, Markus and Klapper, Wolfram and Burkhardt, Birgit and Feller, Alfred C. and Hummel, Michael and Loeffler, Markus and Rosolowski, Maciej and Schwaenen, Carsten and Spang, Rainer and Stein, Harald and Thorns, Christoph and Truemper, Lorenz and Vater, Inga and Wessendorf, Swen and Zenz, Thorsten and Siebert, Reiner and Kueppers, Ralf (2010) Detection of genomic aberrations in molecularly defined Burkitt's lymphoma by array-based, high resolution, single nucleotide polymorphism analysis. HAEMATOLOGICA-THE HEMATOLOGY JOURNAL, 95 (12). pp. 2047-2055. ISSN 0390-6078, 1592-8721
Full text not available from this repository. (Request a copy)Abstract
Background Knowledge about the genetic lesions that occur in Burkitt's lymphoma, besides the pathognomonic IG-MYC translocations, is limited. Design and Methods Thirty-nine molecularly-defined Burkitt's lymphomas were analyzed with high-resolution single-nucleotide polymorphism chips for genomic imbalances and uniparental disomy. Imbalances were correlated to expression profiles and selected micro-RNA analysis. Translocations affecting the MYC locus were studied by fluoresence in situ hybridization. Results We detected 528 copy number changes, defining 29 recurrently imbalanced regions. Five hundred and eighteen regions of uniparental disomy were found, but these were rarely recurrent. Combined imbalance mapping and expression profiling revealed a strong correlation between copy number and expression. Several recurrent imbalances affected the MYC pathway: the micro-RNA-supercluster 17-92 was frequently gained and the transcription factor E2F2 was recurrently deleted. Molecular Burkitt's lymphoma lacking MYC translocations showed MYC gains. Amplifications of the polymerase iota gene were associated with increased frequency of positions scored as aberrant. Conclusions The present findings suggest that uniparental disomies do not play a major role in the pathogenesis of Burkitt's lymphoma, whereas some genes may contribute to the development of this lymphoma through gene dosage effects. Amplifications of the polymerase iota gene may be functionally linked with increased genomic alterations in Burkitt's lymphoma. The pattern and rarity of chromosomal changes detectable, even at the high resolution employed here, together with aberrations of genes regulating MYC activity, support the hypothesis that deregulation of the MYC pathway is the major force driving the pathogenesis of Burkitt's lymphoma, but show that this deregulation is more complex than previously known.
| Item Type: | Article |
|---|---|
| Uncontrolled Keywords: | DNA-POLYMERASE-IOTA; B-CELL LYMPHOMAS; LOSS-OF-HETEROZYGOSITY; COPY-NUMBER; MALIGNANT-LYMPHOMA; EXPRESSION; CANCER; HYBRIDIZATION; GENE; MYC; Burkitt's lymphoma; genomic imbalance; MYC; uniparental disomy |
| Subjects: | 600 Technology > 610 Medical sciences Medicine |
| Divisions: | Medicine > Institut für Funktionelle Genomik > Lehrstuhl für Statistische Bioinformatik (Prof. Spang) |
| Depositing User: | Dr. Gernot Deinzer |
| Date Deposited: | 06 Jul 2020 09:25 |
| Last Modified: | 06 Jul 2020 09:25 |
| URI: | https://pred.uni-regensburg.de/id/eprint/23791 |
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