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首页> 外文期刊>International journal of oncology >Differential BCCIP gene expression in primary human ovarian cancer, renal cell carcinoma and colorectal cancer tissues
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Differential BCCIP gene expression in primary human ovarian cancer, renal cell carcinoma and colorectal cancer tissues

机译:BCCIP基因在人原发性卵巢癌,肾细胞癌和大肠癌组织中的差异表达

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摘要

Human BCCIP, a protein which interacts with BRCA2 and CDKN1A (Cip1, p21), has been implicated in many cellular processes including cell cycle regulation, DNA recombination and damage repair, telomere maintenance, embryonic development and genomic stability. BCCIP gene expression, which is an important BRCA2 cofactor in tumor suppression, has been identified in some primary cancers. Thus, we investigated the role of BCCIP expression in a large sample of clinically diagnosed primary ovarian cancer, renal cell carcinoma (RCC) and colorectal cancer (CRC) tissues. Using clinically diagnosed frozen primary cancer tissues, quantitative PCR (qPCR), western blot analysis (WB) and immunohistochemical staining (IHC) approaches were used to detect and measure gene expression. Reduced BCCIP gene expression in ovarian cancer, RCC and CRC tissues occurred in 74, 89 and 75% of tissue samples, respectively. qPCR analysis of mRNA expression in 54 ovarian cancer, 50?RCC and 44?CRC samples revealed significant (>2-fold decreased) BCCIP downregulation in 56, 70 and 46% of tissue samples, respectively. Although BCCIP expression in three different tumor tissues decreased, the relationship between BCCIP expression and clinicopathological features of each cancer was distinct. Compared to normal tissues, BCCIP expression in ovarian cancers was significantly downregulated in serous, endometrioid and mucinous carcinomas. Downregulation of BCCIP expression was strongly associated with clear cell RCC (ccRCC) and Fuhrman tumor grading, but significant differences in BCCIP expression between CRC and matched normal tissues occurred only in male CRC tissues (p<0.05) and in tissue with a T4 tumor stage (p<0.01). Thus, BCCIP protein was chiefly reduced in ovarian cancer and RCC tissue samples (p<0.05). BCCIP gene expression was downregulated in human ovarian cancer, RCC and CRC tissues, suggesting a role for the gene in the pathogenesis of these cancers.
机译:人BCCIP是一种与BRCA2和CDKN1A相互作用的蛋白质(Cip1,p21),已参与许多细胞过程,包括细胞周期调控,DNA重组和损伤修复,端粒维持,胚胎发育和基因组稳定性。 BCCIP基因表达是在肿瘤抑制中重要的BRCA2辅因子,已在某些原发性癌症中得到鉴定。因此,我们调查了BCCIP表达在大量临床诊断的原发性卵巢癌,肾细胞癌(RCC)和结直肠癌(CRC)组织中的作用。利用临床诊断的冷冻原发癌组织,定量PCR(qPCR),蛋白质印迹分析(WB)和免疫组织化学染色(IHC)方法被用于检测和测量基因表达。 BCCIP基因在卵巢癌,RCC和CRC组织中的表达降低分别在74、89和75%的组织样本中发生。 qPCR分析了54个卵巢癌,50?RCC和44?CRC样品中的mRNA表达,分别显示56、70和46%的组织样品中BCCIP显着下调(> 2倍下降)。尽管在三个不同的肿瘤组织中BCCIP表达下降,但是BCCIP表达与每种癌症的临床病理特征之间的关系是明显的。与正常组织相比,卵巢癌中的BCCIP表达在浆液性,子宫内膜样和黏液性癌中显着下调。 BCCIP表达的下调与透明细胞RCC(ccRCC)和Fuhrman肿瘤分级密切相关,但是CRC与匹配的正常组织之间BCCIP表达的显着差异仅发生在男性CRC组织中(p <0.05)和处于T4肿瘤分期的组织(p <0.01)。因此,BCCIP蛋白在卵巢癌和RCC组织样本中主要减少(p <0.05)。 BCCIP基因表达在人类卵巢癌,RCC和CRC组织中被下调,表明该基因在这些癌症的发病机理中具有重要作用。

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