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Potential role of p53 mutation in chemical hepatocarcinogenesis of rats

机译:p53突变在大鼠化学性肝癌发生中的潜在作用

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摘要

AIM: Inactivation of p53 gene is one of the most frequent genetic alterations in carcinogenesis. The mutation status of p53 gene was analyzed, in order to understand the effect of p53 mutation on chemical hepatocarcinogenesis of rats. METHODS: During hepatocarcinogenesis of rats induced by 3′-methyl-4- dimethylaminoazobenzene (3′-Me-DAB), prehepatocarcinoma and hepatocarcinoma foci were collected by laser capture microdissection (LCM), and quantitatively analyzed for levels of p53 mRNA by LightCycler~(TM) real-time RT-PCR and for mutations in p53 gene exons 5-8 by direct sequencing. RESULTS: Samples consisting of 44 precancerous foci and 24 cancerous foci were collected by LCM. A quantitative analysis of p53 mRNA showed that p53 mRNA peaked at an early stage (week 6) in the prehepatocarcinoma lesion, more than ten times that of adjacent normal tissue, and gradually decreased from week 6 to week 24. The expression of p53 mRNA in adjacent normal tissue was significantly lower than that in prehepatocarcinoma. Similar to prehepatocarcinoma, p53 mRNA in cancer was markedly higher than that in adjacent normal tissue at week 12, and was closer to normal at week 24. Direct p53 gene sequencing showed that 35.3% (24/68) (9 precancer, 15 cancer) LCM samples exhibited point mutations, 20.5% of prehepatocarcinoma LCM samples presented missense mutations at exon 6/7 or/and 8, and was markedly lower than 62.5% of hepatocarcinoma ones (P<0.01). Mutation of p53 gene formed the mutant hot spots at 5 codons. Positive immunostaining for p53 protein could be seen in prehepatocarcinoma and hepatocarcinoma foci at 24 weeks. CONCLUSION: p53 gene mutation is present in initial chemical hepatocarcinogenesis, and the mutation of p53 gene induced by 3′-Me-DAB is an important factor of hepatocarcinogenesis.
机译:目的:p53基因失活是致癌作用中最常见的遗传改变之一。为了了解p53突变对大鼠化学性肝癌发生的作用,分析了p53基因的突变状态。方法:在3'-甲基-4-二甲基氨基偶氮苯(3'-Me-DAB)诱导的大鼠肝癌发生过程中,通过激光捕获显微切割术(LCM)收集肝癌前和肝癌灶,并通过LightCycler〜定量分析p53 mRNA的水平。 (TM)实时RT-PCR并通过直接测序检测p53基因外显子5-8中的突变。结果:LCM收集了44例癌前灶和24例癌灶。对p53 mRNA的定量分析表明,p53 mRNA在肝癌前病变的早期(第6周)达到峰值,是邻近正常组织的十倍以上,并在第6周至第24周逐渐下降。癌旁正常组织明显低于肝癌前组织。与肝癌相似,癌症的p53 mRNA在第12周时显着高于邻近正常组织,在第24周时接近正常。直接p53基因测序显示35.3%(24/68)(9个癌前期,15个癌症) LCM样品表现出点突变,占肝癌前病变的20.5%LCM样品在第6/7或/和8号外显子出现错义突变,明显低于肝癌的62.5%(P <0.01)。 p53基因的突变在5个密码子处形成突变热点。在肝癌前和肝癌灶中,在第24周时可以看到p53蛋白的阳性免疫染色。结论:最初的化学肝癌发生中存在p53基因突变,而3'-Me-DAB诱导的p53基因突变是肝癌发生的重要因素。

著录项

  • 来源
    《World Journal of Gastroenterology》 |2004年第1期|p.46-52|共7页
  • 作者单位

    Department of Nutrition and Food Hygiene, School of Public Health, Jilin University, Changchun 130021, Jilin Province, China;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 消化系及腹部疾病;
  • 关键词

  • 入库时间 2022-08-17 23:37:34

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