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Clinicopathologic parameters associated with the FDG-avidity in staging of early gastric cancer using 18F-FDG PET

机译:使用18F-FDG PET在早期胃癌分期中与FDG亲和力相关的临床病理参数

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摘要

This study investigated the clinicopathologic factors associated with 2-[18F]fluoro-2-deoxy-d-glucose (18F-FDG) uptake of early gastric cancer (EGC) and used them to design a clinical scoring method to predict FDG-avidity of EGC.Two hundred twenty-nine retrospectively enrolled patients underwent preoperative 18F-FDG positron emission tomography/computed tomography (PET/CT). Histologic information was obtained by gastrectomy (n = 195) or endoscopic mucosal dissection (n = 34). The association between clinicopathologic factors and 18F-FDG uptake by the primary tumor was determined. The results were used to develop a clinical scoring method.18F-FDG uptake was detected in 49 (17.5%) patients. According to univariate analysis, location, gross type, World Health Organization classification, Lauren classification, size, depth of invasion, and lymphatic invasion were significant variables affecting 18F-FDG uptake (all P < .05). According to multivariate analysis, location (lower 3rd, P = .035), gross type (0–I, 0–IIa, P < .001), size (≥2.5 cm, P = .026), and depth of invasion (submucosa, P = .007) were significantly associated with FDG-avidity. A clinical scoring system, ranged from 0 to 4, was developed by giving one score to 4 independent variables. A cut-off value of 2.5 showed good prediction of FDG-avidity in EGCs, with a sensitivity and specificity of 65.0% and 85.2%, respectively.18F-FDG uptake by EGC depends on location, gross type, size, and depth of invasion of the primary tumor. A clinical scoring system based on clinicopathologic variables can predict the FDG-avidity of primary tumors in patients with EGC.
机译:本研究调查了早期胃癌(EGC)摄取2-[ 18 F]氟-2-脱氧-d-葡萄糖( 18 F-FDG)相关的临床病理因素),并用它们设计出一种临床评分方法,以预测EGC的FDG亲和力。229例回顾性研究的患者接受了术前 18 F-FDG正电子发射断层扫描/计算机断层扫描(PET / CT) 。通过胃切除术(n = 195)或内窥镜黏膜剥离术(n = 34)获得组织学信息。确定临床病理因素与原发肿瘤摄取 18 F-FDG的关系。该结果用于建立临床评分方法。在49名患者中检测到 18 F-FDG摄入量(17.5%)。根据单因素分析,位置,总体类型,世界卫生组织分类,Lauren分类,大小,浸润深度和淋巴管浸润是影响 18 F-FDG摄取的重要变量(所有P <.05) 。根据多变量分析,位置(下三级,P = .035),总体类型(0-I,0-IIa,P <.001),大小(≥2.5cm,P = .026)和浸润深度(黏膜下层,P = .007)与FDG亲和力显着相关。通过给4个独立变量一个分数,开发了一种临床评分系统,范围从0到4。截止值为2.5可以很好地预测EGC中FDG的抗体亲和力,其敏感性和特异性分别为65.0%和85.2%。 18 EGC摄取F-FDG取决于位置,总原发肿瘤的类型,大小和浸润深度。基于临床病理变量的临床评分系统可以预测EGC患者原发性肿瘤的FDG亲和力。

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