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血吸虫性膀胱癌中p53基因的突变:对92例埃及患者肿瘤的研究以及血吸虫性和非血吸虫性尿路上皮肿瘤突变谱的比较

Mutations in the p53 gene in schistosomal bladder cancer: a study of 92 tumours from Egyptian patients and a comparison between mutational spectra from schistosomal and non-schistosomal urothelial tumours.

作者信息

Warren W, Biggs P J, el-Baz M, Ghoneim M A, Stratton M R, Venitt S

机构信息

Section of Molecular Carcinogenesis, Haddow Laboratories, Royal Cancer Hospital, Sutton, Surrey, UK.

出版信息

Carcinogenesis. 1995 May;16(5):1181-9. doi: 10.1093/carcin/16.5.1181.

Abstract

Much of bladder cancer in East Africa and the Middle East is attributed to chronic urinary infection with Schistosoma haematobium ('schistosomiasis'). Most schistosomal bladder cancer (SBC) is squamous cell carcinoma (SCC) and occurs in the fifth decade of life. In contrast, nonschistosomal bladder cancer (NSBC) in Western countries usually occurs in the seventh decade of life and is largely transitional cell carcinoma (TCC). To shed light on the mechanisms underlying these different patterns of bladder cancer we looked for mutations in the p53 gene in SBC from 92 patients in Egypt, where schistosomiasis is hyperendemic. Patients' mean age at presentation of bladder cancer was 49.4 +/- 9.9 years and 90% had a clinical history of schistosomiasis and/or histological evidence of schistosomal eggs adjacent to the carcinoma. There were 53 SCC, 23 TCC, 13 adenocarcinomas and three other carcinomas. Thirty patients had tumours with mutations in exons 5-8 of the p53 gene: 17/53 SCC, 8/23 TCC, 4/13 adenocarcinomas and 1/3 other tumours. Of 19 mutations in SCC, 16 were base pair substitutions (BPS), two were deletions and one an insertion. Two tumours each contained two mutations. Of the BPS, nine were transitions at CpG dinucleotides and two were G-->T transversions. All the mutations in TCC were BPS: four were transitions at CpG dinucleotides and three were G-->C transversions. One TCC had two mutations. Of four adenocarcinomas with mutations, two had transitions at CpG dinucleotides. Of the 30 BPS mutations, 16 were transitions at CpG dinucleotides, of which 12 were C-->T. We combined these 33 mutations with six obtained from Egyptian SCC reported by Habuchi et al. (Cancer Res., 53, 3795-3799, 1993) to compile a mutational spectrum. This was compared with a NSBC spectrum assembled from 118 mutations reported in the literature. The proportion of BPS at CpG dinucleotides was significantly higher in SBC than in NSBC (18/34 versus 25/103, P = 0.003). There was also a bias away from mutations in exons 7 and 8 towards mutations in exons 5 and 6. We suggest that the excess of transitions at CpG dinucleotides in SBC results from nitric oxide (NO) produced by the inflammatory response provoked by schistosomal eggs. NO could produce such mutations directly, by deamination of 5-methylcytosine, and indirectly, following conversion to nitrate, bacterial reduction to nitrite and endogenous formation of urinary N-nitroso compounds. These produce O6-alkylguanines in DNA, leading to very high rates of G:C-->A:T transitions, a process possibly augmented by inefficient repair of alkylated bases at CpG dinucleotides.

摘要

东非和中东地区的许多膀胱癌都归因于感染埃及血吸虫(“血吸虫病”)导致的慢性尿路感染。大多数血吸虫性膀胱癌(SBC)是鳞状细胞癌(SCC),发病于人生的第五个十年。相比之下,西方国家的非血吸虫性膀胱癌(NSBC)通常发病于人生的第七个十年,且主要是移行细胞癌(TCC)。为了深入了解这些不同膀胱癌模式背后的机制,我们对埃及92例SBC患者的p53基因进行了突变检测,埃及是血吸虫病高度流行地区。患者患膀胱癌时的平均年龄为49.4±9.9岁,90%有血吸虫病临床病史和/或癌旁组织学血吸虫卵证据。其中有53例SCC、23例TCC、13例腺癌和3例其他类型癌症。30例患者的肿瘤p53基因外显子5 - 8存在突变:17/53例SCC、8/23例TCC、4/13例腺癌和1/3例其他肿瘤。在SCC的19个突变中,16个是碱基对替换(BPS),2个是缺失突变,1个是插入突变。2个肿瘤各有2个突变。在BPS中,9个是CpG二核苷酸处的转换突变,2个是G→T颠换突变。TCC中的所有突变都是BPS:4个是CpG二核苷酸处的转换突变,3个是G→C颠换突变。1例TCC有2个突变。在4例有突变的腺癌中,2例是CpG二核苷酸处的转换突变。在30个BPS突变中,16个是CpG二核苷酸处的转换突变,其中12个是C→T。我们将这33个突变与Habuchi等人(《癌症研究》,53卷,3795 - 3799页,1993年)报道的埃及SCC的6个突变合并,编制了一个突变谱。并将其与从文献报道的118个突变汇总而成的NSBC谱进行比较。SBC中CpG二核苷酸处BPS的比例显著高于NSBC(18/34对25/103,P = 0.003)。而且存在一种从外显子7和8的突变向外显子5和6的突变的偏向性。我们认为,SBC中CpG二核苷酸处转换突变过多是由血吸虫卵引发的炎症反应产生的一氧化氮(NO)导致的。NO可通过5 - 甲基胞嘧啶脱氨直接产生此类突变,也可在转化为硝酸盐、细菌还原为亚硝酸盐以及内源性形成尿N - 亚硝基化合物后间接产生。这些物质在DNA中产生O6 - 烷基鸟嘌呤,导致G:C→A:T转换的发生率非常高,这一过程可能因CpG二核苷酸处烷基化碱基修复效率低下而加剧。

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