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Role and limitation of FMPSPGR dynamic contrast scanning in the follow—up of patients with hepatocellular carcinoma treated by TACE
作者姓名:Yan FH  Zhou KR  Cheng JM  Wang JH  Yan ZP  Da RR  Fan J  Ji Y
作者单位:Fu-Hua Yan,Kang-Rong Zhou,Jie-Min Cheng,Jian-Hua Wang,Zhi-Ping Yan,Reng-Rong Da(Department of Radiology, Zhongshan Hospital, Fudan University, Shanghai 200032, China);Jia Fan(Departnent of Hepatobiliary-surgery, Zhongshan Hospital,Fudan University, Shanghai 200032, China);Yuan Ji(Department of Pathology, Zhongshan Hospital, Fudan University, Shanghai 200032, China) 
基金项目:卫生部临床学科重点项目 
摘    要:AIM:To evaluate the role and limitation of fast multiplanar spoiled gradient-recalled(FMPSPGR)MRdynamiccontrast scanning in the follow-up of patients with HCCtreated by transarterial chemoembolization(TACE).METHODS:Twenty-two patients with 24HCClesions confirmed by biopsy or surgical resection underwent MR imaging in 4-9wks after TACEwith a superconducting 1.5TMR scanner,including SE T1WI,T2WIand FMPSPGR dynamic contrast scanning.The signal intensities of all lesions on SET1WI,T2WIand the enhancement patterns on FMPSPGRdynamic contrast scanning were observed,and the comparison was made between MRI findings and pathological results in all the casese.RESULTS:Of the 24lesions,the signal intensities were various on SET1WIand T2WI.OnT1WI,13lesions appeared as hyperintense,4 lesions were isointense and the other 7lesions were hypointensese,Histologically.Hyperintense lesions showed on T1WI were viable tumor or hemorrhage;isointensities were coagulative necrosis or inflammatory infiltration;hypointensities were tumor,liquified necrosis,coagulative necrosis or inflammatory infiltration.OnT2WI,15lesions appeared as hyperintense,3lesions were isointense and the other 6lesions were hypointensese,Hyperintense lesions shower on T2WI were residuals of viable tumor,hemorrhage,liquefied necrosis or inflammatory infiltration;isointense lesions were residuals of viable tumor or inflammatory infiltration;hypointense lesions were coagulative necrosis.On FMPSPGR dynamic contrast scanning,18 of the 24lesions enhanced on early-phase dynamic scanning corresponding to residuals of viable tumor and the other 6lesions had no enhancement at this phase because complete necrosis were seen in the histologic examination.On delayed-phase dynamic scanning,6lesions had permanent enhancement appeared as inhomogeneous hyperintensity and both residuals of viable tumor and inflammatory infiltration were found by histologic examination,18 lesions were hypointense at this phase and 8of them coexisted with peripheral ring-like enhancement of the lesions resulting from viable tumors or inflammatory infiltration.CONCLUSION:FMPSPGR MR dynamic contrast scanning can reflect the pathologic changes of HCCtreated by TACE.Especially.early-phase dynamic scanning can evaluate accurately residuals of viable tumor and necrosis in HCClesions.FMPSPGR dynamic contrast scanning is useful in the follow-up of patients with HCC treated by TACEcombined with SET1WIand T2WI,but is is difficult to differentiate peripheral viable tumors from inflammatory infiltration.

关 键 词:肝癌  肝动脉栓塞化疗术  FMPSPGR  辅助治疗  有效性  临床研究
收稿时间:2001 Dec 5

Role and limitation of FMPSPGR dynamic contrast scanning in the follow-up of patients with hepatocellular carcinoma treated by TACE
Yan FH,Zhou KR,Cheng JM,Wang JH,Yan ZP,Da RR,Fan J,Ji Y.Role and limitation of FMPSPGR dynamic contrast scanning in the follow-up of patients with hepatocellular carcinoma treated by TACE[J].World Journal of Gastroenterology,2002,8(4):658-662.
Authors:Yan Fu-Hua  Zhou Kang-Rong  Cheng Jie-Min  Wang Jian-Hua  Yan Zhi-Ping  Da Reng-Rong  Fan Jia  Ji Yuan
Institution:1. Department of Radiology, Zhongshan Hospital, Fudan University, Shanghai 200032, China
2. Departnent of Hepatobiliary-surgery, Zhongshan Hospital,Fudan University, Shanghai 200032, China
3. Department of Pathology, Zhongshan Hospital, Fudan University, Shanghai 200032, China
Abstract:AIM: To evaluate the role and limitation of fast multiplanar spoiled gradient-recalled (FMPSPGR) MR dynamic contrast scanning in the follow-up of patients with HCC treated by transarterial chemoembolization (TACE). METHODS: Twenty-two patients with 24 HCC lesions confirmed by biopsy or surgical resection underwent MR imaging in 4-9wks after TACE with a superconducting 1.5 T MR scanner, including SE T(1)WI, T(2)WI and FMPSPGR dynamic contrast scanning. The signal intensities of all lesions on SE T(1)WI,T(2)WI and the enhancement patterns on FMPSPGR dynamic contrast scanning were observed, and the comparison was made between MRI findings and pathological results in all the cases. RESULTS: Of the 24 lesions, the signal intensities were various on SE T(1)WI and T(2)WI. On T(1)WI, 13 lesions appeared as hyperintense, 4 lesions were isointense and the other 7 lesions were hypointensese. Histologically, hyperintense lesions showed on T(1)WI were viable tumor or hemorrhage; isointensities were coagulative necrosis or inflammatory infiltration; hypointensities were tumor, liquified necrosis, coagulative necrosis or inflammatory infiltration. On T(2)WI, 15 lesions appeared as hyperintense, 3 lesions were isointense and the other 6 lesions were hypointensese. Hyperintense lesions showed on T(2)WI were residuals of viable tumor, hemorrhage, liquefied necrosis or inflammatory infiltration; isointense lesions were residuals of viable tumor or inflammatory infiltration; hypointense lesions were coagulative necrosis. On FMPSPGR dynamic contrast scanning, 18 of the 24 lesions enhanced on early-phase dynamic scanning corresponding to residuals of viable tumor and the other 6 lesions had no enhancement at this phase because complete necrosis were seen in the histologic examination. On delayed-phase dynamic scanning, 6 lesions had permanent enhancement appeared as inhomogeneous hyperintensity and both residuals of viable tumor and inflammatory infiltration were found by histologic examination. 18 lesions were hypointense at this phase and 8 of them coexisted with peripheral ring-like enhancement of the lesions resulting from viable tumors or inflammatory infiltration. CONCLUSION: FMPSPGR MR dynamic contrast scanning can reflect the pathologic changes of HCC treated by TACE. Especially, early-phase dynamic scanning can evaluate accurately residuals of viable tumor and necrosis in HCC lesions. FMPSPGR dynamic contrast scanning is useful in the follow-up of patients with HCC treated by TACE combined with SE T(1)WI and T(2)WI, but it is difficult to differentiate peripheral viable tumors from inflammatory infiltration.
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