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Diagnostic value of negative enrichment and immune fluorescence in situ hybridization for intraperitoneal free cancer cells of gastric cancer

摘要Objective:To explore the intraperitoneal free cancer cell (IFCC) detection value of negative enrichment and immune fluorescence in situ hybridization (NEimFISH) on chromosomes (CEN) 8/17.Methods:To verify the reliability of NEimFISH,29 gastric cancer tumors,their adjacent tissues and greater omental tissues were tested.Our study then included 105 gastric cancer patents for IFCC.We defined patients as IFCC-positive if a signal was detected,regardless of the detailed cancer cell numbers.A comparison of clinicopathological features was conducted among IFCC groups.We also compared the diagnosis value and peritoneal recurrence predictive value among different detection methods.The comparison of IFCC number was also conducted among different groups.Results:A cutoff of 2.5 positive cells could distinguish all benign tissue samples and 97% of malignant tissue samples in our study.Compared to intestinal gastric cancer,patients with diffuse gastric cancer tended to have more IFCCs (6 vs.4,P=0.002).The IFCC counts were often higher in the lymphovascular invasion positive group than negative group (3 vs.1,P=0.022).All IFCC samples that were considered positive using conventional cytology were also found to be positive using NEimFISH.When compared to conventional cytology and paraffin pathology,NEimFISH had a higher IFCC positive rate (68.9%) and higher one-year peritoneal recurrence predictive value with area under the curve (AUC) of 0.922.Conclusions:Gastric cancer could be effectively diagnosed by NEimFISH.The IFCC number found using NEimFISH on CEN8/17 is closely associated with Lauren type and vascular invasion of cancer.NEimFISH is a reliable detection modality with a higher positive detection rate,higher one-year peritoneal recurrence predictive value and quantitative features for IFCC of gastric cancer.

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作者单位 Key Laboratory of Carcinogenesis and Translational Research(Ministry of Education/Beijing), Center of Gastrointestinal Surgery, Peking University Cancer Hospital & Institute, Beijing 100142, China [1] Key Laboratory of Carcinogenesis and Translational Research(Ministry of Education/Beijing), Department of Pathology, Peking University Cancer Hospital & Institute, Beijing 100142, China [2] Cyttel Biosciences INC,Taizhou 225316, China [3] Key Laboratory of Carcinogenesis and Translational Research(Ministry of Education/Beijing), Clinical Laboratory,Peking University Cancer Hospital & Institute, Beijing 100142, China [4]
栏目名称 Original Article
DOI 10.21147/j.issn.1000-9604.2019.06.10
发布时间 2020-04-29
基金项目
This study was supported by the National Science Foundation for Young Scientists of China
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中国癌症研究(英文版)

中国癌症研究(英文版)

2019年31卷6期

945-954页

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