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首页> 外文期刊>NeuroImage: Clinical >Diffusivity in multiple sclerosis lesions: At the cutting edge?
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Diffusivity in multiple sclerosis lesions: At the cutting edge?

机译:多发性硬化症病变的扩散性:在最前沿?

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Background Radial Diffusivity (RD) has been suggested as a promising biomarker associated with the level of myelination in MS lesions. However, the level of RD within the lesion is affected not only by loss of myelin sheaths, but also by the degree of tissue destruction. This may lead to exaggeration of diffusivity measures, potentially masking the effect of remyelination. Objective To test the hypothesis that the T2 hyperintense lesion edge that extends beyond the T1 hypointense lesion core is less affected by tissue loss, and therefore a more appropriate target for imaging biomarker development targeting de- and re-myelination. Method Pre- and post-gadolinium (Gd) enhanced T1, T2 and DTI images were acquired from 75 consecutive RRMS patients. The optic radiation (OR) was identified in individual patients using a template-based method. T2 lesions were segmented into T1-hypointense and T1-isointense areas and lesion masks intersected with the OR. Average Radial, Axial and Mean diffusivity (RD, AD and MD) and fractional anisotropy (FA) were calculated for lesions of the entire brain and the OR. In addition, Gd enhancing lesions were excluded from the analysis. Results 86% of chronic T2 lesions demonstrated hypointense areas on T1-weighted images, which typically occupied the central part of each T2 lesion, taking about 40% of lesional volume. The T1-isointense component of the T2 lesion was most commonly seen as a peripheral ring of relatively constant thickness (“T2-rim”). While changes of diffusivity between adjacent normal appearing white matter and the “T2-rim” demonstrated a disproportionally high elevation of RD compare to AD, the increase of water diffusion was largely isointense between the “T2-rim” and T1-hypointense parts of the lesion. Conclusion Distinct patterns of diffusivity within the central and peripheral components of MS lesions suggest that axonal loss dominates in the T1 hypointense core. The effects of de/remyelination may be more readily detected in the “T2-rim”, where there is relative preservation of structural integrity. Identifying and separating those patterns has an important implication for clinical trials of both neuroprotective and, in particular, remyelinating agents. Highlights ? Distinct patterns of diffusivity within the central and peripheral components of MS lesions were identified. ? Axonal loss is likely to dominate the T1 hypointense core. ? The effects of de/remyelination may be more readily detected in the “T2-rim”.
机译:背景放射扩散(RD)被认为是与MS病变的髓鞘形成有关的有前途的生物标志物。然而,病变内RD的水平不仅受到髓鞘的损失,而且还受到组织破坏程度的影响。这可能会导致扩散措施的夸张,可能掩盖了髓鞘再生的作用。目的为了检验以下假设:延伸到T1低点病变核心之外的T2高强度病变边缘受组织损失的影响较小,因此是针对脱髓鞘和再髓鞘形成的生物标志物显影进行成像的更合适的靶点。方法从75名连续的RRMS患者中获取了d前后的T1,T2和DTI增强图像。使用基于模板的方法在单个患者中确定了光辐射(OR)。 T2病变被分为T1低点和T1等强度区域,病变面膜与OR相交。计算整个大脑和手术室病变的平均径向,轴向和平均扩散率(RD,AD和MD)和分数各向异性(FA)。另外,从分析中排除了增强Gd的病变。结果86%的慢性T2病变在T1加权图像上显示低点区域,通常占据每个T2病变的中心部分,约占病变体积的40%。 T2病变的T1等强度成分最常被视为厚度相对恒定的外围环(“ T2边缘”)。尽管相邻的正常出现的白质和“ T2-边缘”之间的扩散率变化显示RD与AD相比不成比例地升高了RD,但水扩散的增加​​在该区域的“ T2-边缘”和T1-低密度部分之间是等强度的。病变。结论MS病变的中央和周边成分的扩散模式不同,提示轴突丢失在T1低点核心占主导。在具有相对完整性的结构完整性的“ T2-rim”中,更容易检测到脱髓鞘/髓鞘再生的作用。识别和分离这些模式对于神经保护剂,尤其是髓鞘再生剂的临床试验具有重要意义。强调 ? MS病变的中央和外围成分内的扩散模式不同。 ?轴突损失很可能占T1低氧核心的主导地位。 ?在“ T2-rim”中可以更容易地检测到脱髓鞘/髓鞘再生的作用。

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