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Utility and limitations of glypican-3 expression for the diagnosis of hepatocellular carcinoma at both ends of the differentiation spectrum

机译:Glypican-3表达在分化谱两端诊断肝细胞癌中的效用和局限性

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Glypican-3 is a heparin sulfate proteoglycan normally expressed in fetal liver and placenta, but not in normal adult liver. Preliminary studies have shown that glypican-3 can be useful for the diagnosis of hepatocellular carcinoma. We performed immunohistochemistry for glypican-3 on 80 resection cases of hepatocellular lesions to examine the utility of glypican-3 immunohistochemistry in hepatocellular carcinoma at two ends of the differentiation spectrum. Staining was compared to Hep Par 1 in poorly differentiated cases. Glypican-3 was expressed in 46 (79%) hepatocellular carcinomas (56, 83 and 89% of well, moderately and poorly differentiated respectively) and seven (64%) fibrolamellar carcinomas. Of the 16 well differentiated cases, 10 closely resembled adenoma and were diagnosed due to focal abnormalities and/or loss of reticulin. Glypican-3 expression was seen in 50% in this group. Hepatocellular carcinomas arising in cirrhotic liver were more likely to be glypican-3 positive (91 vs 57%, P=0.004). All hepatic adenomas and macroregenerative nodules were negative, and three (43%) high grade dysplastic nodules were positive. Focal staining was seen in regenerative nodules in four (11%) cirrhosis cases. Glypican-3 was significantly more sensitive than Hep Par 1 for diagnosis of poorly differentiated hepatocellular carcinomas (89 vs 63%, P=0.02). The difference was more significant when only cases with diffuse positive staining were considered (83 vs 21%, P<0.001). In conclusion, glypican-3 has high sensitivity for the diagnosis of hepatocellular carcinoma, but is less sensitive in the extremely well differentiated hepatocellular carcinoma and fibrolamellar variant of hepatocellular carcinoma. Caution should be exercised in using glypican-3 in biopsy specimens as cirrhotic nodules can show strong expression. Glypican-3 can be especially useful in the identification of poorly differentiated hepatocellular carcinoma as it has higher sensitivity compared to Hep Par 1.
机译:Glypican-3是一种硫酸肝素蛋白聚糖,通常在胎儿肝脏和胎盘中表达,但在正常成人肝脏中不表达。初步研究表明,glypican-3可用于诊断肝细胞癌。我们对80例肝细胞病变切除病例中的glypican-3进行了免疫组化分析,以研究glypican-3免疫组化在肝癌分化谱的两端的作用。在低分化病例中将染色与Hep Par 1进行比较。 Glypican-3在46(79%)的肝细胞癌中表达(分别分化为分别良好分化,中度和低分化的56%,83%和89%)和7种(64%)的纤维状薄层癌。在16例分化良好的病例中,有10例非常类似于腺瘤,并由于病灶异常和/或网状蛋白丢失而被诊断出。在该组中观察到50%的Glypican-3表达。肝硬化肝中发生的肝细胞癌更有可能是Glypican-3阳性(91比57%,P = 0.004)。所有肝腺瘤和大体再生结节均为阴性,三个(43%)高级别增生性结节为阳性。在4例(11%)肝硬化病例中,再生结节可见病灶染色。 Glypican-3对Hep Par 1诊断低分化肝细胞癌的敏感性显着更高(89 vs 63%,P = 0.02)。当仅考虑弥散阳性染色的病例时,差异更为显着(83%vs 21%,P <0.001)。总之,glypican-3对肝细胞癌的诊断具有较高的敏感性,但对分化程度极高的肝细胞癌和肝细胞纤维状变体的敏感性较低。在肝活检标本中应谨慎使用glypican-3,因为肝硬化结节可表现出强表达。 Glypican-3在鉴定低分化肝细胞癌中尤其有用,因为它比Hep Par 1具有更高的敏感性。

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