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作 者:文泽军[1] 史大鹏[1] 朱绍成[1] 魏毅[1]
出 处:《实用放射学杂志》2016年第7期1066-1069,1084,共5页Journal of Practical Radiology
基 金:国家重点专科建设项目(国卫办医函[2013]544号).
摘 要:目的:探讨睾丸生殖细胞肿瘤的 MRI 表现,提高对该疾病的 MRI 诊断水平。方法回顾性分析经手术病理证实的25例睾丸生殖细胞肿瘤患者临床及 MRI 资料,所有病例均行 MRI 平扫,其中16例行动态 MRI 增强扫描。利用 MRI 对睾丸肿瘤的大小、形态、信号特点、毗邻关系、强化方式及肿瘤血管情况进行评估,并与病理对照。结果25例睾丸生殖细胞肿瘤中,精原细胞瘤10例,其中 T2 WI 呈均匀低信号8例,稍低信号2例,增强扫描轻度结节样强化5例,明显均匀强化2例,其中4例可见纤维间隔强化;卵黄囊瘤4例,T1 WI 呈等低信号,T2 WI 呈稍高信号,增强扫描后肿瘤呈渐进式强化;成熟型畸胎瘤、表皮样囊肿、混合性生殖细胞肿瘤各3例,T1 WI 呈混杂低信号,T2 WI 呈混杂高信号;胚胎性癌2例,T1 WI 呈等低信号,T2 WI 呈混杂低信号,其内可见出血信号,增强扫描呈分隔强化。结论MRI 对睾丸生殖细胞肿瘤诊断正确率较高,对其病理分型、分期及鉴别诊断具有重要价值。Objective To explore the imaging characteristics of testicular germ cell tumors and to improve the MRI diagnostic level. Methods MRI and clinical data of 25 cases confirmed testicular germ cell tumor by pathological examination were retrospectively analyzed. All the 25 cases were performed plain scan of MRI,and 16 patients underwent MRI enhanced scan.The size,morphology,signal intensity, adjacent structures,enhancement figure and tumor supplying artery were assessed and the histopathological findings were servered as the standard of reference.Results In the all 25 testicular germ cell tumors,10 cases were seminoma,8 cases showed homogeneous low signal intensity,2 cases of seminoma were low signal intensity on T2 WI,furthermore 5 cases performed poor nodular enhance-ment,2 cases performed homogeneous enhancement,4 cases performed fibrous septa enhancement.4 cases were yolk sac tumor ap-peared equal-low signal on T1 WI,slightly high signal intensity on T2 WI and progressive enhancement.Mature teratoma,pidermoid cyst and mixed germ cell tumor were 3 cases respectively,the MRI demonstrated mixed low signal intensity on T1 WI and mixed high signal on T2 WI.2 cases were embryonal carcinoma demonstrated middle-low signal intensity on T1 WI,and mixed low signal intensity on T2 WI.The two cases revealed bleeding signal intensity and septa enhancement.Conclusion MRI can be used to diagnose germ cell tumors with high accuracy,and provides essential information for pathological type,stage and differential diagnosis.
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