首页> 外文期刊>Digestive and liver disease: official journal of the Italian Society of Gastroenterology and the Italian Association for the Study of the Liver >Contrast-enhanced computed tomography and ultrasound-guided liver biopsy to diagnose dysplastic liver nodules in cirrhosis
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Contrast-enhanced computed tomography and ultrasound-guided liver biopsy to diagnose dysplastic liver nodules in cirrhosis

机译:对比增强计算机断层扫描和超声引导下的肝活检诊断肝硬化中增生的肝结节

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Background: Dysplastic nodules in cirrhosis herald a very high risk of transition to hepatocellular carcinoma. A better understanding of the relationships between dysplastic nodules and hepatocellular carcinoma development may help refining strategies of enhanced follow-up. Methods: All consecutive cirrhotics with a histologically proven de novo dysplastic nodule, were retrospectively identified and underwent alternating abdominal ultrasound and contrast-computed tomography every 3 months. An ultrasound-guided liver biopsy was the diagnostic gold standard, whereas surveillance and recall policies were according to current guidelines. Results: Among 36 patients with dysplastic nodule (21 low-grade, 15 high-grade, 17.4±2.6 mm), 17 (47%) showed arterial wash-in, 15 (42%) portal/venous hypodensity whereas 4 (11%) had neither pattern. During 6-128 (median 36) months, 21 patients developed a hepatocellular carcinoma at a rate of 13.8% per year, intranodular. =8.7% vs extranodular. =7.1% per year. Hepatocellular carcinoma occurred more frequently in high-grade than low-grade dysplastic nodules (32.2% vs 9.3% per year, p=0.0039); the maximum time to hepatocellular carcinoma transformation was 27 months for intranodular vs 67 months for extranodular tumours (p=0.025). No contrast-computed tomography pattern predicted neoplastic transformation of dysplastic nodules. Conclusion: The histological examination of liver nodules in cirrhosis lacking the imaging hallmark of hepatocellular carcinoma improves both prognostication and outcome of surveillance, since it dictates the intensity of the radiological follow-up.
机译:背景:肝硬化中的增生性结节预示着向肝细胞癌转化的风险很高。更好地了解增生性结节与肝细胞癌发展之间的关系可能有助于改善随访策略。方法:回顾性鉴定所有经组织学证实为新发增生性结节的肝硬化患者,每3个月进行交替的腹部超声检查和对比计算机断层扫描。超声引导的肝活检是诊断的金标准,而监视和召回政策是根据当前指南进行的。结果:在36例增生性结节患者中(21例低度,15例高度,17.4±2.6 mm),其中17例(47%)表现为动脉冲洗,15例(42%)门/静脉低密度,而4例(11%) )都没有模式。在6-128(中位数36)个月内,有21例结节内发生肝细胞癌,每年发生率为13.8%。 = 8.7%vs结节外每年= 7.1%。高级别肝细胞癌的发生率高于低级别不典型增生性结节(每年32.2%比9.3%,p = 0.0039);结节内肝癌转化的最长时间为27个月,结节外肿瘤为67个月(p = 0.025)。没有对比计算机断层扫描模式预测增生性结节的肿瘤转变。结论:缺乏肝细胞癌影像学特征的肝硬化肝结节的组织学检查可改善预后和监测结果,因为它决定了影像学随访的强度。

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