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Oncogenic Properties of Candidate Oncogenes in Chromosome Region 17p11.2p12 in Human Osteosarcoma

机译:人骨肉瘤染色体区域17p11.2p12中候选致癌基因的致癌特性

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摘要

Osteosarcomas are primary tumors of bone that most often develop in adolescents. They are characterized by complex genomic changes including amplifications, deletions, and translocations. The chromosome region 17p11.2p12 is frequently amplified in human high grade osteosarcomas (25% of cases), suggesting the presence of one or more oncogenes. In previous studies, we identified 9 candidate oncogenes in this region (GID4, ARGHAP44, LRRC75A-AS1, TOP3A, COPS3, SHMT1, PRPSAP2, PMP22, and RASD1). The aim of the present study was to determine their oncogenic properties. Therefore, we generated osteosarcoma cell lines overexpressing these genes, except for LRRC75A-AS1 and PRPSAP2, and subjected these to functional oncogenic assays. We found that TOP3A, SHMT1, and RASD1 overexpression provided increased proliferation and that ARGHAP44, COPS3, and PMP22 overexpression had a stimulatory effect on migration and invasion of the cells. COPS3 and PMP22 overexpression additionally improved the ability of the cells to form new colonies. No oncogenic effect could be demonstrated for GID4 overexpression. We conclude that the concerted amplification-mediated overexpression of these genes in 17p11.2p12 may contribute to the oncogenic process in malignant osteosarcoma. (C) 2016 S. Karger AG, Basel
机译:骨肉瘤是最常见于青少年的原发性骨肿瘤。它们的特征是复杂的基因组变化,包括扩增,缺失和易位。染色体区域17p11.2p12在人类高度骨肉瘤中经常扩增(25%的病例),表明存在一种或多种癌基因。在以前的研究中,我们确定了该区域的9种候选癌基因(GID4,ARGHAP44,LRRC75A-AS1,TOP3A,COPS3,SHMT1,PRPSAP2,PMP22和RASD1)。本研究的目的是确定其致癌特性。因此,我们生成了除LRRC75A-AS1和PRPSAP2以外的过表达这些基因的骨肉瘤细胞系,并对其进行了功能致癌分析。我们发现TOP3A,SHMT1和RASD1的过表达提供了增加的增殖,而ARGHAP44,COPS3和PMP22的过表达对细胞的迁移和侵袭具有刺激作用。 COPS3和PMP22的过表达还提高了细胞形成新菌落的能力。没有证据表明GID4过表达具有致癌作用。我们得出结论,这些基因在17p11.2p12中的协同扩增介导的过表达可能有助于恶性骨肉瘤的致癌过程。 (C)2016 S.Karger AG,巴塞尔

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