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扩散加权成像与可变翻转角T1映射:肝纤维化随访分析中图像引导活检的补充手段

Diffusion-weighted imaging and variable flip angle T1 mapping: a supplement for image-guided biopsy in follow-up analysis of liver fibrosis.

作者信息

Hu Peng, Sun Jihong, Lv Fangfang, Pi Borui, Xu Fangping, Han Guocan, Hu Xi, Wang Yue, Huang Ning, Wu Xia, Yang Xiaoming

机构信息

Department of Radiology, Sir Run Run Shaw Hospital, Zhejiang University School of Medicine, Hangzhou City 310016, Zhejiang Province, China.

Department of Infectious Diseases, Sir Run Run Shaw Hospital, Zhejiang University School of Medicine, Hangzhou City 310016, Zhejiang Province, China.

出版信息

J Interv Med. 2019 Apr 30;1(3):150-156. doi: 10.19779/j.cnki.2096-3602.2018.03.04. eCollection 2018 Aug.

Abstract

To evaluate the performance of diffusion-weighted imaging (DWI) and variable flip angle (VFA) T1 mapping as a supplement to image-guided biopsy in follow-up analysis of liver fibrosis. This prospective study was approved by the institution's committee on human research, and written informed consent was provided from the enrolled patients. We investigated five MRI parameters of DWI and VFA T1 mapping, collected from 11 patients who underwent serial ultrasound image-guided biopsy with follow-up MRI within 1.5 years after treatment for liver fibrosis/cirrhosis. For each patient, four consecutive MRI examinations were conducted, including baseline MRI before treatment and three follow-up MRI examinations after treatment at each 0.5-year interval. ADC values at four b values and T1 relaxation times were correlated to pathology-confirmed liver fibrosis stages, which were subsequently divided into two groups, stages F2-3 and F4. The receiver operating characteristic (ROC) analysis and repeated measurement analysis of variance were used for statistical analysis. Among these ADC parameters, ADC value (b = 500 s/mm) was the most consistent in differentiating between stage F2-3 and F4 liver fibrosis. Repeated measurement analysis showed that the intra-group and inter-group differences were 0.447 and 0.024, respectively. T1 relaxation time could not consistently differentiate between the F2-3 and F4 groups; however, it was repeatable, and the intra-group and inter-group differences were 0.410 and 0.042, respectively. MRI-ADC value at a b value of 500 s/mm can be a promising biomarker for differentiating stages F2-3 and F4 liver fibrosis. A combination of this biomarker with repeatable T1 relaxation time may function as a non-invasive tool for follow-up liver fibrosis in patients who reject repeated image-guided biopsy.

摘要

评估扩散加权成像(DWI)和可变翻转角(VFA)T1映射在肝纤维化随访分析中作为图像引导活检补充手段的性能。这项前瞻性研究经机构人类研究委员会批准,已获得纳入患者的书面知情同意书。我们研究了DWI和VFA T1映射的五个MRI参数,这些参数来自11例接受肝纤维化/肝硬化治疗后1.5年内接受系列超声图像引导活检及随访MRI检查的患者。对于每位患者,进行了四次连续的MRI检查,包括治疗前的基线MRI以及治疗后每隔0.5年的三次随访MRI检查。四个b值下的表观扩散系数(ADC)值和T1弛豫时间与病理证实的肝纤维化分期相关,随后将其分为两组,即F2 - 3期和F4期。采用受试者操作特征(ROC)分析和重复测量方差分析进行统计分析。在这些ADC参数中,ADC值(b = 500 s/mm²)在区分F2 - 3期和F4期肝纤维化方面最为一致。重复测量分析表明,组内差异和组间差异分别为0.447和0.024。T1弛豫时间不能始终如一地区分F2 - 3组和F4组;然而,它具有可重复性,组内差异和组间差异分别为0.410和0.042。b值为500 s/mm²时的MRI - ADC值可能是区分F2 - 3期和F4期肝纤维化的一种有前景的生物标志物。这种生物标志物与具有可重复性的T1弛豫时间相结合,可能成为拒绝重复图像引导活检患者肝纤维化随访的一种非侵入性工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7392/8586563/2ce97fc62641/gr1.jpg

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