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在通过3号染色体片段转移进行基因改造的新型卵巢癌细胞系模型中,对与肿瘤抑制相关的3p12.3-pcen区域的特征分析。

Characterization of the 3p12.3-pcen region associated with tumor suppression in a novel ovarian cancer cell line model genetically modified by chromosome 3 fragment transfer.

作者信息

Cody Neal A L, Shen Zhen, Ripeau Jean-Sebastien, Provencher Diane M, Mes-Masson Anne-Marie, Chevrette Mario, Tonin Patricia N

机构信息

Department of Human Genetics, McGill University, Montreal, Quebec, Canada H3A 1A4.

出版信息

Mol Carcinog. 2009 Dec;48(12):1077-92. doi: 10.1002/mc.20535.

Abstract

The genetic analysis of nontumorigenic radiation hybrids generated by transfer of chromosome 3 fragments into the tumorigenic OV-90 ovarian cancer cell line identified the 3p12.3-pcen region as a candidate tumor suppressor gene (TSG) locus. In the present study, polymorphic microsatellite repeat analysis of the hybrids further defined the 3p12.3-pcen interval to a 16.1 Mb common region containing 12 known or hypothetical genes: 3ptel-ROBO2-ROBO1-GBE1-CADM2-VGLL3-CHMP2B-POU1F1-HTR1F-CGGBP1-ZNF654-C3orf38-EPHA3-3pcen. Seven of these genes, ROBO1, GBE1, VGLL3, CHMP2B, CGGBP1, ZNF654, and C3orf38, exhibited gene expression in the hybrids, placing them as top TSG candidates for further analysis. The expression of all but one (VGLL3) of these genes was also detected in the parental OV-90 cell line. Mutations were not identified in a comparative sequence analysis of the predicted protein coding regions of these candidates in OV-90 and donor normal chromosome 3 contig. However, the nondeleterious sequence variants identified in the transcribed regions distinguished parent of origin alleles for ROBO1, VGLL3, CHMP2B, and CGGBP1 and cDNA sequencing of the hybrids revealed biallelic expression of these genes. Interestingly, underexpression of VGLL3 and ZNF654 were observed in malignant ovarian tumor samples as compared with primary cultures of normal ovarian surface epithelial cells or benign ovarian tumors, and this occurred regardless of allelic content of 3p12.3-pcen. The results taken together suggest that dysregulation of VGLL3 and/or ZNF654 expression may have affected pathways important in ovarian tumorigenesis which was offset by the transfer of chromosome 3 fragments in OV-90, a cell line hemizygous for 3p.

摘要

通过将3号染色体片段转移至致瘤性OV - 90卵巢癌细胞系而产生的非致瘤性辐射杂种细胞的遗传分析,确定3p12.3 - pcen区域为候选肿瘤抑制基因(TSG)位点。在本研究中,对杂种细胞的多态性微卫星重复分析进一步将3p12.3 - pcen区间限定到一个16.1 Mb的共同区域,该区域包含12个已知或假设的基因:3ptel - ROBO2 - ROBO1 - GBE1 - CADM2 - VGLL3 - CHMP2B - POU1F1 - HTR1F - CGGBP1 - ZNF654 - C3orf38 - EPHA3 - 3pcen。这些基因中的7个,即ROBO1、GBE1、VGLL3、CHMP2B、CGGBP1、ZNF654和C3orf38,在杂种细胞中表现出基因表达,使其成为进一步分析的顶级TSG候选基因。除了一个基因(VGLL3)外,这些基因在亲本OV - 90细胞系中也均有表达。在对OV - 90和供体正常3号染色体重叠群中这些候选基因的预测蛋白质编码区域进行的比较序列分析中,未发现突变。然而,在转录区域鉴定出的非有害序列变异区分了ROBO1、VGLL3、CHMP2B和CGGBP1的亲本来源等位基因,并且杂种细胞的cDNA测序显示这些基因的双等位基因表达。有趣的是,与正常卵巢表面上皮细胞的原代培养物或良性卵巢肿瘤相比,在恶性卵巢肿瘤样本中观察到VGLL3和ZNF654的表达下调,并且这种情况与3p12.3 - pcen的等位基因含量无关。综合这些结果表明,VGLL3和/或ZNF654表达失调可能影响了卵巢肿瘤发生中重要的途径,而这在3p半合子的细胞系OV - 90中被3号染色体片段的转移所抵消。

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