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Sodium MRI in Multiple Sclerosis is Compatible with Intracellular Sodium Accumulation and Inflammation-Induced Hyper-Cellularity of Acute Brain Lesions

机译:多发性硬化症中的钠MRI与急性脑病变的细胞内钠积累和炎症诱导的超细胞性兼容

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摘要

The cascade of inflammatory pathogenetic mechanisms in multiple sclerosis (MS) has no specific conventional MRI correlates. Clinicians therefore stipulate improved imaging specificity to define the pathological substrates of MS in vivo including mapping of intracellular sodium accumulation. Based upon preclinical findings and results of previous sodium MRI studies in MS patients we hypothesized that the fluid-attenuated sodium signal differs between acute and chronic lesions. We acquired brain sodium and proton MRI data of N = 29 MS patients; lesion type was defined by the presence or absence of contrast enhancement. N = 302 MS brain lesions were detected, and generalized linear mixed models were applied to predict lesion type based on sodium signals; thereby controlling for varying numbers of lesions among patients and confounding variables such as age and medication. Hierarchical model comparisons revealed that both sodium signals average tissue (χ2(1) = 27.89, p < 0.001) and fluid-attenuated (χ2(1) = 5.76, p = 0.016) improved lesion type classification. Sodium MRI signals were significantly elevated in acute compared to chronic lesions compatible with intracellular sodium accumulation in acute MS lesions. If confirmed in further studies, sodium MRI could serve as biomarker for diagnostic assessment of MS, and as readout parameter in clinical trials promoting attenuation of chronic inflammation.
机译:多发性硬化症(MS)中的炎症致病机制的级联没有特定的常规MRI相关性。因此,临床医生规定改进的成像特异性以定义体内MS的病理学底物,包括绘制细胞内钠积累的图谱。基于临床前的发现以及先前在MS患者中进行钠MRI研究的结果,我们假设急性和慢性病变的体液衰减钠信号有所不同。我们获得了N = 29 MS患者的脑钠和质子MRI数据;病变类型由是否存在造影剂增强定义。检测N = 302 MS脑部病变,并应用广义线性混合模型基于钠信号预测病变类型。从而控制患者中不同数量的病变,并混淆诸如年龄和药物治疗等变量。分层模型比较显示,钠信号平均组织(χ 2 (1)= 27.89,p <0.001)和体液衰减(χ 2 (1)= 5.76, p = 0.016)改善了病变类型分类。与与急性MS病变中细胞内钠积累相容的慢性病变相比,急性MRI钠信号显着升高。如果在进一步的研究中得到证实,钠MRI可以作为诊断MS的生物标记物,并在临床试验中作为促进慢性炎症减轻的读出参数。

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