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定量T1对多发性硬化症中的皮质髓鞘再生敏感:一项死后MRI研究。

Quantitative T1 is sensitive to cortical remyelination in multiple sclerosis: A postmortem MRI study.

作者信息

Galbusera Riccardo, Weigel Matthias, Bahn Erik, Schaedelin Sabine, Cagol Alessandro, Lu Po-Jui, Barakovic Muhamed, Melie-Garcia Lester, Franz Jonas, Dechent Peter, Nair Govind, Kappos Ludwig, Brück Wolfgang, Stadelmann Christine, Granziera Cristina

机构信息

Translational Imaging in Neurology (ThINk) Basel, Department of Biomedical Engineering, Faculty of Medicine, University Hospital Basel and University of Basel, Basel, Switzerland.

Department of Neurology, University Hospital Basel, Basel, Switzerland.

出版信息

Brain Pathol. 2025 Sep;35(5):e70010. doi: 10.1111/bpa.70010. Epub 2025 Apr 14.

Abstract

Remyelination of cortical lesions in people with multiple sclerosis (pwMS) has been shown to be extensive. In this work, we aimed to assess whether postmortem quantitative MRI (qMRI) can help detect those areas. We imaged six fixed whole brains of deceased pwMS by 3T-MRI using magnetization transfer ratio (MTR, 570 μm isotropic), myelin water fraction (MWF, 1000 μm isotropic), quantitative T1 (qT1, 670 μm isotropic), quantitative susceptibility mapping (QSM, 330 μm isotropic) and radial diffusivity (RD, 1300 or 1400 μm isotropic) maps. Immunohistochemistry for myelin proteins was performed in 129 tissue blocks including the cortex and enabled the detection of cortical demyelination (DM), cortical remyelination (RM), and normal-appearing cortex (NAC). We identified 25 DM, 25 RM, and for each of these areas, a corresponding NAC near the lesion. Wilcoxon paired tests showed that: (a) qT1 and RD were higher and QSM lower in DM versus NAC (all p < 0.001), whereas RD was higher and QSM lower in RM versus NAC (p = 0.048 and p < 0.01 respectively); (b) mean qT1 in RM did not differ from mean qT1 in NAC (p = 0.074); (c) MWF and MTR were not different between DM and RM. We compared the delta between DM versus NAC (∆DM) and the delta between RM versus NAC (∆RM) using a Mann-Whitney test, in which RM showed a partial recovery of qT1 only (∆qT1 DM > ∆qT1 RM, p = 0.045). Mixed-effect models confirmed the findings obtained using univariate analyses. qT1 and QSM, but not RD, correlated with MBP intensity (r = -0.28, p < 0.01 and r = 0.29, p < 0.01 respectively). A Bonferroni correction was performed for multiple testing. Our data show that qT1 is altered in demyelinated but not in remyelinated cortical areas, while QSM and RD are affected by any cortical abnormalities. Accordingly, qT1 might be considered a potential imaging biomarker of cortical RM.

摘要

多发性硬化症患者(pwMS)皮质病变的再髓鞘化已被证明是广泛的。在这项研究中,我们旨在评估尸检定量磁共振成像(qMRI)是否有助于检测这些区域。我们使用3T磁共振成像对6例已故pwMS患者的固定全脑进行成像,采用了磁化传递率(MTR,各向同性分辨率570μm)、髓磷脂水分数(MWF,各向同性分辨率1000μm)、定量T1(qT1,各向同性分辨率670μm)、定量磁化率成像(QSM,各向同性分辨率330μm)和径向扩散率(RD,各向同性分辨率1300或1400μm)图谱。对包括皮质在内的129个组织块进行了髓磷脂蛋白的免疫组织化学检测,从而能够检测皮质脱髓鞘(DM)、皮质再髓鞘化(RM)和外观正常的皮质(NAC)。我们确定了25个DM区域、25个RM区域,并为这些区域中的每一个确定了病变附近相应的NAC区域。Wilcoxon配对检验表明:(a)与NAC相比,DM区域的qT1和RD更高,QSM更低(所有p<0.001),而与NAC相比,RM区域的RD更高,QSM更低(分别为p = 0.048和p<0.01);(b)RM区域的平均qT1与NAC区域相比无差异(p = 0.074);(c)DM和RM之间的MWF和MTR无差异。我们使用Mann-Whitney检验比较了DM与NAC之间的差值(∆DM)和RM与NAC之间的差值(∆RM),其中RM仅显示qT1部分恢复(∆qT1 DM>∆qT1 RM,p = 0.045)。混合效应模型证实了单变量分析的结果。qT1和QSM与髓磷脂碱性蛋白(MBP)强度相关,但RD不相关(r分别为-0.28,p<0.01和r = 0.29,p<0.01)。对多重检验进行了Bonferroni校正。我们的数据表明,qT1在脱髓鞘的皮质区域发生改变,但在再髓鞘化的皮质区域未改变,而QSM和RD受到任何皮质异常的影响。因此,qT1可能被认为是皮质RM的潜在成像生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8532/12352926/5651ae4411b8/BPA-35-e70010-g002.jpg

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