Itoi T, Takei K, Shinohara Y, Takeda K, Nakamura K, Horibe T, Sanada A, Ohno H, Matsubayashi H, Saito T, Watanabe H
Fourth Department of Internal Medicine, Tokyo Medical College, Japan.
Pathol Int. 1999 Jan;49(1):30-7. doi: 10.1046/j.1440-1827.1999.00821.x.
To evaluate whether it is useful for diagnosis to detect K-ras and p53 mutations in biopsy specimens and bile of biliary tract lesions, 12 cholangiocarcinomas (CC), eight cases of cholangitis, seven gallbladder carcinomas (GBC), seven gallbladder cholesterol polyps, four cases of adenomyomatosis of the gallbladder and five cases of cholecystitis were examined. K-ras and p53 mutations in bile were detected by a two-step polymerase chain reaction (PCR) and nested PCR-single-strand conformation polymorphism (SSCP) analysis. In addition, p53 protein expression in biopsy specimens from CC were examined by immunostaining. K-ras mutations at codon 12 were detected in 50% of CC and 57.1% of GBC in both biopsy specimens and bile. The incidence of p53 mutations was 33.3% in CC and 42.9% in GBC. p53 protein overexpression was observed in 60% CC biopsy specimens. In contrast, K-ras and p53 abnormalities were not detected in any non-neoplastic biliary tract lesion. K-ras and p53 mutations in biliary tract cancers showed the same mutation patterns in spite of differences in the collection methods used between bile and biopsy specimens or surgically resected tissue. Genetic analysis of K-ras and p53 mutations in biopsy specimens and bile may be useful for the diagnosis of biliary tract cancers, although it may be effectively limited to patients with advanced disease.
为评估检测胆道病变活检标本及胆汁中的K-ras和p53突变对诊断是否有用,我们对12例胆管癌(CC)、8例胆管炎、7例胆囊癌(GBC)、7例胆囊胆固醇息肉、4例胆囊腺肌增生症及5例胆囊炎进行了检测。采用两步聚合酶链反应(PCR)及巢式PCR-单链构象多态性(SSCP)分析检测胆汁中的K-ras和p53突变。此外,通过免疫染色检测CC活检标本中的p53蛋白表达。在活检标本及胆汁中,50%的CC和57.1%的GBC检测到第12密码子的K-ras突变。CC中p53突变发生率为33.3%,GBC中为42.9%。60%的CC活检标本中观察到p53蛋白过表达。相反,在任何非肿瘤性胆道病变中均未检测到K-ras和p53异常。尽管胆汁与活检标本或手术切除组织的采集方法不同,但胆道癌中的K-ras和p53突变显示出相同的突变模式。活检标本及胆汁中K-ras和p53突变的基因分析可能有助于胆道癌的诊断,尽管可能仅限于晚期疾病患者。
