7q deletion mapping and expression profiling in uterine fibroids

被引:0
|
作者
Sakari Vanharanta
Noel C Wortham
Päivi Laiho
Jari Sjöberg
Kristiina Aittomäki
Johanna Arola
Ian P Tomlinson
Auli Karhu
Diego Arango
Lauri A Aaltonen
机构
[1] University of Helsinki,Department of Medical Genetics
[2] Biomedicum Helsinki,Department of Obstetrics and Gynaecology
[3] Molecular and Population Genetics Laboratory,Department of Clinical Genetics
[4] Cancer Research UK,Department of Pathology
[5] Helsinki University Central Hospital,undefined
[6] Helsinki University Central Hospital,undefined
[7] University of Helsinki,undefined
来源
Oncogene | 2005年 / 24卷
关键词
fibroid; oligonucleotide microarray; gene expression; chromosome 7; loss of heterozygosity; tumour suppressor gene;
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学科分类号
摘要
Uterine fibroids are some of the most common tumours of females, but relatively little is known about their molecular basis. Several studies have suggested that deletions on chromosome 7q could have a role in fibroid formation. We analysed 165 sporadic uterine fibroids to define a small 3.2 megabase (Mb) commonly deleted region on 7q22.3–q31.1, flanked by clones AC005070 and AC007567. We also used oligonucleotide microarrays to compare the expression profiles of 10 samples of normal myometrium and 15 fibroids, nine of which displayed 7q-deletions. Activating transcription factor 3, patched homolog (Drosophila), homeo box A5, death-associated protein kinase 1, and retinoic acid receptor responder 3 were downregulated, and excision repair crosscomplementing 3, transcription factor AP-2 gamma and protein kinase C beta 1 were upregulated in fibroids. New pathways were discovered related to fibroid formation. The presence or absence of 7q-deletions did not dramatically affect the global expression pattern of the tumours; changes, however, were observed in genes related to vesicular transport and nucleic acid binding.
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页码:6545 / 6554
页数:9
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