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Suspicious brush cytology is an indication for liver transplantation evaluation in primary sclerosing cholangitis

机译:可疑刷细胞学检查可作为原发性硬化性胆管炎肝移植评估的指标

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摘要

AIM To investigate markers for high-grade dysplasia for the optimal timing of liver transplantation in patients with primary sclerosing cholangitis (PSC). METHODS Earlier data support a dysplasia-carcinoma sequence, even low-to high-grade dysplasia, in PSC-associated cholangiocarcinoma (CCA). Surveillance using endoscopic retrograde cholangiography (ERC) and brush cytology aims to detect cases of biliary dysplasia, and liver transplantation is an option in cases with suspicion of malignancy in brushing. This study investigated markers to identify patients with high-grade biliary dysplasia for optimal timing in early liver transplantation. Patients undergoing surveillance using ERC and brush cytology during 2008-2014 and who were diagnosed with biliary dysplasia in explanted liver or CCA until February 2016 were included in the study. Demographic data, cholangiography findings, laboratory values, cytological morphology and DNA ploidy were analysed. RESULTS Thirty PSC patients had biliary neoplasia in the explanted liver during the study period. Sixteen of these patients had low-grade dysplasia, 10 patients had high-grade dysplasia, and 4 patients had CCA. Fifteen PSC patients diagnosed with CCA were not transplanted. Patients with low-grade dysplasia were younger. Alkaline phosphatase or carcinoembryonic antigen values did not differ between groups during surveillance, but carbohydrate antigen 19-9 was higher in CCA patients. No difference in PSC duration, ERC scores, suspicious cytology, or ploidy analysis was found between groups. No difference was observed between fibrosis stage in explanted livers. Low-and high-grade dysplasia could not be differentiated before liver transplantation based on liver enzymes, tumour markers, ERC scores, brush cytology or DNA ploidy. CONCLUSION Repeated suspicion of neoplasia in brush cytology should be an indication for evaluations of liver transplantation prior to the development of CCA.
机译:目的探讨用于原发性硬化性胆管炎(PSC)患者肝移植最佳时机的高度不典型增生的标志物。方法较早的数据支持与PSC相关的胆管癌(CCA)的异型增生-癌序列,甚至从低到高程度的异型增生。使用内窥镜逆行胆管造影术(ERC)和刷细胞学进行监测旨在发现胆道发育不良的病例,如果怀疑刷牙有恶性肿瘤,则可以选择肝移植。这项研究调查了标记物,以鉴定患有严重胆管异型增生的患者,以便在早期肝移植中获得最佳时机。该研究纳入了在2008年至2014年期间使用ERC和笔刷细胞学进行监视的患者,并在2016年2月之前被诊断出肝或CCA的胆道发育异常。分析了人口统计学数据,胆管造影结果,实验室值,细胞学形态和DNA倍性。结果在研究期间,有30例PSC患者在外植肝脏中有胆道肿瘤。这些患者中有16例患有低度不典型增生,10例患有高度不典型增生,4例患有CCA。 15名被诊断为CCA的PSC患者未移植。低度不典型增生的患者较年轻。监测期间两组间的碱性磷酸酶或癌胚抗原值无差异,但CCA患者的碳水化合物抗原19-9较高。在两组之间,PSC持续时间,ERC评分,可疑细胞学检查或倍性分析均无差异。在移植肝的纤维化阶段之间未观察到差异。肝移植前不能根据肝脏酶,肿瘤标志物,ERC评分,刷细胞学或DNA倍性来区分低度和高度异型增生。结论在刷细胞学中反复怀疑肿瘤形成,应作为评估CCA发生前肝移植评估的指标。

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