Glypican-3和甲胎蛋白作为肝细胞癌的诊断试验。

Jorge Filmus, Mariana Capurro
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引用次数: 62

摘要

肝细胞癌是最常见的恶性肿瘤之一。它通常在早期无症状,往往是血管内和胆道内侵入。因此,大多数患者在发现HCC时表现为不治之症,早期诊断对于预后良好至关重要。小肿瘤的影像学诊断相对不准确,因为肝硬化和发育不良结节在影像学上与HCC相似。因此,找到一种合适的血清学标志物来区分HCC和良性肝脏病变,将对早期诊断非常有用。目前唯一广泛用于HCC诊断的血清学标志物是甲胎蛋白(AFP)。然而,该标志物的敏感性有限(41-65%)。鉴于HCC的高度异质性,目前认为,HCC的最佳血清学检测将基于同时测量两种或三种高度特异性的血清学标志物。几个实验室最近报道,glypican-3 (GPC3)是一种膜结合蛋白多糖,在大部分hcc中表达,但在正常肝细胞和非恶性肝病中检测不到。此外,多项研究表明GPC3可作为HCC患者的血清学检测。虽然该检测在慢性肝病人群中特异性非常高,但敏感性有限(与AFP在同一范围内)。有趣的是,在大多数情况下,GPC3值升高与AFP值升高无关。结果,在绝大多数HCC患者中,这两种标志物中至少一种的血清学水平升高。这些结果表明,在不影响特异性的情况下,同时测量GPC3和AFP的诊断试验的敏感性可以显著提高。
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Glypican-3 and alphafetoprotein as diagnostic tests for hepatocellular carcinoma.

Hepatocellular carcinoma (HCC) is one of the most common types of malignant tumor. It is usually asymptomatic in the early stages and tends to be intravascularly and intrabiliary invasive. Therefore, most patients present with incurable disease at the time of detection and early diagnosis of HCC is critical for a good prognosis. The imaging-based diagnosis of small tumors is relatively inaccurate, as cirrhotic and dysplastic nodules mimic HCC radiologically. The availability of a suitable serological marker to distinguish between HCC and benign liver lesions would, therefore, be very useful for early diagnosis. The only serological marker currently widely used for the diagnosis of HCC is alphafetoprotein (AFP). However, the sensitivity of this marker is limited (41-65%). Given the high heterogeneity of HCC, it is currently thought that an optimal serological test for HCC will be based on the simultaneous measurement of two or three highly specific serological markers.Several laboratories have recently reported that glypican-3 (GPC3), a membrane-bound proteoglycan, is expressed by a large proportion of HCCs, but is undetectable in normal hepatocytes and non-malignant liver disease. Furthermore, various studies demonstrated that GPC3 could be used as a serological test for the diagnosis of patients with HCC. Although the specificity of the test was very high in the context of a population with chronic liver disease, the sensitivity was limited (within the same range as AFP). Interestingly, in most cases, elevated GPC3 values did not correlate with elevated AFP values. As a consequence, the serological level of at least one of the two markers was elevated in a large majority of HCC patients. These results suggest that the sensitivity of the diagnostic test can be significantly improved without compromising specificity with the simultaneous measurement of both GPC3 and AFP.

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