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肝细胞腺瘤、局灶性结节性增生、肝硬化及肝细胞癌中的p53免疫反应性

p53 immunoreactivity in hepatocellular adenoma, focal nodular hyperplasia, cirrhosis and hepatocellular carcinoma.

作者信息

Ojanguren I, Ariza A, Castellà E M, Fernández-Vasalo A, Mate J L, Navas-Palacios J J

机构信息

Department of Anatomic Pathology, Hospital Universitari Germans Trias i Pujol, Barcelona, Spain.

出版信息

Histopathology. 1995 Jan;26(1):63-8. doi: 10.1111/j.1365-2559.1995.tb00622.x.

Abstract

The prolonged half-life of mutant p53 makes feasible its immunocytochemical detection. In order to assess the pathogenetic role of mutant p53 in regenerative and neoplastic liver disease we studied its immunohistochemical expression in cases of hepatic cirrhosis, hepatocellular carcinoma (HCC), cirrhosis with areas of HCC, hepatocellular adenoma and focal nodular hyperplasia. The study included needle and wedge biopsies of 50 cirrhotic livers, 59 HCCs (36 of them with associated cirrhosis), six adenomas and two focal nodular hyperplasias. Sixty-five HCC fine-needle cytology specimens were also included in the study. There was no immunohistochemical evidence of mutant p53 expression in any of the cases of cirrhotic liver (except for one instance associated with HCC) adenoma or focal nodular hyperplasia. In contrast p53 was detected in 8.5% of HCC cases in the biopsy series and 24% of HCC cases in the fine needle aspiration series. In addition, mutant p53 expression in HCC was positively correlated with tumour grade. According to grade, the distribution of p53 positive immunoreactivity among HCCs was as follows: Grade I-II, 0% of cases in the biopsy series and 9% in the fine needle aspirates; Grade III, 18% in the biopsy series and 55% in the fine needle aspirates; and Grade IV, 40% in the biopsy series. Therefore, mutant p53 expression does not seem to be associated with benign liver lesions but seems to correlate with the progression of HCC through various grades of increasing malignancy.

摘要

突变型p53的半衰期延长使得其免疫细胞化学检测成为可能。为了评估突变型p53在再生性和肿瘤性肝病中的致病作用,我们研究了其在肝硬化、肝细胞癌(HCC)、伴有HCC区域的肝硬化、肝细胞腺瘤和局灶性结节性增生病例中的免疫组化表达。该研究包括50例肝硬化肝脏、59例HCC(其中36例伴有相关肝硬化)、6例腺瘤和2例局灶性结节性增生的针吸活检和楔形活检。该研究还纳入了65例HCC细针细胞学标本。在任何肝硬化肝脏病例(除1例与HCC相关的病例外)、腺瘤或局灶性结节性增生中均未发现突变型p53表达的免疫组化证据。相比之下,在活检系列中8.5%的HCC病例和细针穿刺系列中24%的HCC病例检测到p53。此外,HCC中突变型p53表达与肿瘤分级呈正相关。根据分级,HCC中p53阳性免疫反应性的分布如下:I-II级,活检系列中0%的病例,细针穿刺中9%的病例;III级,活检系列中18%的病例,细针穿刺中55%的病例;IV级,活检系列中40%的病例。因此,突变型p53表达似乎与良性肝脏病变无关,但似乎与HCC通过不同程度的恶性进展相关。

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