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p53 密码子 248(外显子 7)与北印度人群膀胱癌风险的关联。

Association of p53 codon 248 (exon7) with urinary bladder cancer risk in the North Indian population.

机构信息

Department of Urology and Renal Transplantation Sanjay Gandhi Post Graduate Institute of Medical Sciences, Lucknow, Uttar Pradesh, India.

出版信息

Biosci Trends. 2011;5(5):205-10. doi: 10.5582/bst.2011.v5.5.205.

DOI:10.5582/bst.2011.v5.5.205
PMID:22101376
Abstract

p53 is the most frequently mutated gene in all forms of human cancer. It responds to diverse stresses including UVR-induced DNA damage and regulates many downstream genes to initiate cell-cycle arrest, DNA repair or apoptosis. p53 gene variants at codon 11, Pro47Ser and codon 248 (exon 7) were evaluated for bladder cancer (BC) risk in North Indians. In the present study, the above encoding regions in p53 genes were analyzed in a hospital based study in 200 BC and 200 healthy controls age and gender matched and of similar ethnicity. The genotyping was assessed by the polymerase chain reaction restriction fragment length polymorphism technique and statistically evaluated using SPSS software ver. 15.0. A significant association was found with p53 codon 248 polymorphism and BC risk whereas p53 codon 11 and p53 Pro47Ser polymorphism showed no association with BC risk. The individuals carrying the heterozygous genotype (Arg/Trp-Arg/Gln) in the p53 codon 248 polymorphism showed high BC risk (p < 0.001). Combinations with heterozygous and variant genotypes also showed a high risk for BC (p < 0.001). The minor allele (Trp/Gln) carriers of the p53 codon 248 demonstrated a 1.7-fold risk for BC. Furthermore, haplotype analysis revealed that the Glu-Pro-Trp/Gln haplotype is associated with a 1.9-fold risk for BC. A protective role was observed with tumor stage/grade of BC patients with p53 codon 248 (p = 0.003; OR = 0.32). Thus, it is evident from our study that of all the 3 single nucleotide polymorphisms evaluated, only p53 codon 248 (exon7) gene polymorphism has an implication for risk in BC in the North Indian population.

摘要

p53 是所有人类癌症中最常发生突变的基因。它对多种应激作出反应,包括 UVR 诱导的 DNA 损伤,并调节许多下游基因以启动细胞周期停滞、DNA 修复或细胞凋亡。在本研究中,在基于医院的研究中分析了 200 名膀胱癌(BC)患者和 200 名年龄和性别匹配且具有相似种族的健康对照者的 p53 基因 11 号密码子、Pro47Ser 和 248 号密码子(外显子 7)的变体。使用聚合酶链反应限制性片段长度多态性技术评估基因分型,并使用 SPSS 软件版本 15.0 进行统计学评估。发现 p53 密码子 248 多态性与 BC 风险显著相关,而 p53 密码子 11 和 p53 Pro47Ser 多态性与 BC 风险无关。在 p53 密码子 248 多态性中携带杂合基因型(Arg/Trp-Arg/Gln)的个体具有较高的 BC 风险(p<0.001)。杂合和变异基因型的组合也显示出较高的 BC 风险(p<0.001)。p53 密码子 248 的次要等位基因(Trp/Gln)携带者患 BC 的风险增加 1.7 倍。此外,单体型分析显示 Glu-Pro-Trp/Gln 单体型与 BC 的风险增加 1.9 倍相关。p53 密码子 248 的 BC 患者肿瘤分期/分级观察到保护作用(p=0.003;OR=0.32)。因此,从我们的研究中可以明显看出,在所评估的所有 3 个单核苷酸多态性中,只有 p53 密码子 248(外显子 7)基因多态性与北印度人群的 BC 风险有关。

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