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首页> 外文期刊>Human Pathology >Quantitative fibrosis estimation by image analysis predicts development of decompensation, composite events and defines event-free survival in chronic hepatitis B patients
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Quantitative fibrosis estimation by image analysis predicts development of decompensation, composite events and defines event-free survival in chronic hepatitis B patients

机译:通过图像分析定量纤维化估计预测了慢性乙型肝炎患者的不良生存率的发育

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The extent of fibrosis is a major determinant of the clinical outcome in patients with chronic liver diseases. We undertook this study to explore the degree of fibrosis in baseline liver biopsies to predict clinical outcomes in chronic hepatitis B (CHB) patients. Fibrosis quantification was done by image analysis on Masson's trichrome stained sections and correlated with clinical and biochemical parameters, liver stiffness and hepatic vein pressure gradient (n = 96). Follow-up information collected related to clinical outcome. A total of 964 cases was analyzed. Median quantitative fibrosis (QF) was 3.7% (interquartile range, 1.6%-9.7%) with substantial variation in various stages. Median QF was FO, 1% (0.7%-1.65%); Fl, 3.03% (2.07%-4.0%); F2, 7.1% (5.6%-8.7%); F3, 12.7% (10.15%-16.7%); F4, 26.9% (20.3%-36.4%). QF positively correlated with METAVIR staging, liver stiffness measurement, and hepatic vein pressure gradient. Eighty-nine cases developed liver-related events: decompensation, hepatocellular carcinoma, liver transplantation and death. Cox regression analysis after adjusting for METAVIR staging QF, albumin, and AST for composite events; QF and albumin for decompensation; and only QF for hepatocellular carcinoma were found to be significant predictors of clinical outcomes. QF categorized into five stages: QF1, 0%-5%; QF2, 5.1%-10%; QF3, 10.1%-15%; QF4, 15.1%-20%; QF5, >20.1%. In patients with advanced stages of QF, probability of event-free survival found to be low. Quantitative fibrosis in baseline liver biopsy predicts progression of the disease and disease outcome in CHB patients. QF defines the probability of event-free survival in CHB cases. (C) 2016 Elsevier Inc. All rights reserved.
机译:纤维化程度是慢性肝病患者临床结果的主要决定因素。我们进行了这项研究,探讨了基线肝脏活组织检查纤维化程度,以预测慢性乙型肝炎(CHB)患者的临床结果。通过对马隆的血管染色部分进行图像分析来进行纤维化定量,并与临床和生化参数,肝刚度和肝静脉压梯度相关(n = 96)。收集的后续信息与临床结果相关。共分析了964例。中值定量纤维化(QF)为3.7%(四分位数,1.6%-9.7%),各个阶段的变化很大。中位数QF是FO,1%(0.7%-1.65%); FL,3.03%(2.07%-4.0%); F2,7.1%(5.6%-8.7%); F3,12.7%(10.15%-16.7%); F4,26.9%(20.3%-36.4%)。 QF与Metavir分期,肝僵硬度测量和肝静脉压力梯度正相关。八十九种病例开发了肝脏相关的事件:失代偿,肝细胞癌,肝移植和死亡。 Cox回归分析调整Metavir分期QF,白蛋白和AST进行复合事件; qf和白蛋白用于失代偿;并且仅发现肝细胞癌的QF是临床结果的显着预测因子。 QF分为五个阶段:QF1,0%-5%; QF2,5.1%-10%; QF3,10.1%-15%; QF4,15.1%-20%; QF5,> 20.1%。在QF QF先进阶段的患者中,发现无事证存活率的可能性很低。基线肝活检中的定量纤维化预测CHB患者疾病和疾病结果的进展。 QF定义CHB病例中无事项存活的概率。 (c)2016年Elsevier Inc.保留所有权利。

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