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通过单链构象多态性(SSCP)凝胶电泳检测p53突变。放射性和非放射性银染SSCP分析的比较研究。

Detection of p53 mutations by single-strand conformation polymorphisms (SSCP) gel electrophoresis. A comparative study of radioactive and nonradioactive silver-stained SSCP analysis.

作者信息

Bosari S, Marchetti A, Buttitta F, Graziani D, Borsani G, Loda M, Bevilacqua G, Coggi G

机构信息

Department of Pathology, University of Milan School of Medicine, Italy.

出版信息

Diagn Mol Pathol. 1995 Dec;4(4):249-55. doi: 10.1097/00019606-199512000-00004.

Abstract

p53 mutations are the most common genetic abnormality in humans tumors, but their clinical significance remains to be precisely elucidated. Conventional single-strand conformation polymorphism (SSCP) analysis, a well-established technique for detecting p53 mutations, uses radioactively labeled polymerase chain reaction (PCR) products, which migrate abnormally in the presence of mutations. We performed radioactive PCR-SSCP analysis in a series of 30 formalin-fixed, paraffin-embedded ovarian carcinomas and two cell lines (SW480 and Caov4) harboring known homozygous p53 mutations and compared the results with nonradioactive silver-stained SSCP. The purpose was to assess whether nonradioactive SSCP is suitable for detecting p53 mutations in a rapid, sensitive, cost-effective fashion, without the need of radioactive isotopes. We accomplished PCR amplification of p53 exons 5 through 8 in 26 carcinomas, and radioactive SSCP detected p53 mutations in 13 tumors; three mutations were localized in exon 5, six in exon 6, two in exon 7, and two in exon 8. All mutations were correctly identified with nonradioactive SSCP, except for one exon 8 mutation. To establish the sensitivity of nonradioactive SSCP, DNA samples of SW480 and Caov4 were mixed with increasing amounts (0-90%) of normal DNA and subjected to PCR-SSCP analysis. Mutations were detected until the concentration of SW480 and Caov4 was 15% and 10%, respectively, of the total sample. The results of our investigation demonstrate that nonradioactive silver-stained SSCP is a sensitive, rapid, and simple technique to detect p53 mutations, even in formalin-fixed tissues, and could be easily used to investigate large series of patients to assess the clinical significance of p53 mutations in human tumors.

摘要

p53 突变是人类肿瘤中最常见的基因异常,但它们的临床意义仍有待精确阐明。传统的单链构象多态性(SSCP)分析是一种成熟的检测 p53 突变的技术,它使用放射性标记的聚合酶链反应(PCR)产物,这些产物在存在突变时会异常迁移。我们对一系列 30 例福尔马林固定、石蜡包埋的卵巢癌以及两个携带已知纯合 p53 突变的细胞系(SW480 和 Caov4)进行了放射性 PCR-SSCP 分析,并将结果与非放射性银染 SSCP 进行比较。目的是评估非放射性 SSCP 是否适合以快速、灵敏、经济高效的方式检测 p53 突变,而无需使用放射性同位素。我们在 26 例癌组织中完成了 p53 外显子 5 至 8 的 PCR 扩增,放射性 SSCP 在 13 个肿瘤中检测到 p53 突变;3 个突变位于外显子 5,6 个位于外显子 6,2 个位于外显子 7,2 个位于外显子 8。除了一个外显子 8 突变外,所有突变均被非放射性 SSCP 正确鉴定。为确定非放射性 SSCP 的灵敏度,将 SW480 和 Caov4 的 DNA 样本与逐渐增加量(0 - 90%)的正常 DNA 混合,并进行 PCR-SSCP 分析。分别直到 SW480 和 Caov4 的浓度占总样本的 15%和 10%时仍能检测到突变。我们的研究结果表明,非放射性银染 SSCP 是一种灵敏、快速且简单的检测 p53 突变的技术,即使在福尔马林固定的组织中也是如此,并且可轻松用于研究大量患者,以评估 p53 突变在人类肿瘤中的临床意义。

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