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Potential of Sodium MRI as a Biomarker for Neurodegeneration and Neuroinflammation in Multiple Sclerosis

机译:钠MRI作为多发性硬化症神经退行性变和神经炎症的生物标记物的潜力

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摘要

In multiple sclerosis (MS), experimental and ex vivo studies indicate that pathologic intra- and extracellular sodium accumulation may play a pivotal role in inflammatory as well as neurodegenerative processes. Yet, in vivo assessment of sodium in the microenvironment is hard to achieve. Here, sodium magnetic resonance imaging (23NaMRI) with its non-invasive properties offers a unique opportunity to further elucidate the effects of sodium disequilibrium in MS pathology in vivo in addition to regular proton based MRI. However, unfavorable physical properties and low in vivo concentrations of sodium ions resulting in low signal-to-noise-ratio (SNR) as well as low spatial resolution resulting in partial volume effects limited the application of 23NaMRI. With the recent advent of high-field MRI scanners and more sophisticated sodium MRI acquisition techniques enabling better resolution and higher SNR, 23NaMRI revived. These studies revealed pathologic total sodium concentrations in MS brains now even allowing for the (partial) differentiation of intra- and extracellular sodium accumulation. Within this review we (1) demonstrate the physical basis and imaging techniques of 23NaMRI and (2) analyze the present and future clinical application of 23NaMRI focusing on the field of MS thus highlighting its potential as biomarker for neuroinflammation and -degeneration.
机译:在多发性硬化症(MS)中,实验和离体研究表明,病理性细胞内和细胞外钠积累可能在炎症以及神经退行性过程中起关键作用。然而,在体内很难评估微环境中的钠。在这里,钠磁共振成像( 23 NaMRI)具有无创性,除了常规的基于质子的MRI外,还提供了一个独特的机会来进一步阐明钠不平衡在体内MS病理学中的作用。但是,钠离子的不利物理特性和体内低浓度导致低信噪比(SNR)以及低空间分辨率(导致部分体积效应)限制了 23 NaMRI的应用。随着最近的高场MRI扫描仪和更先进的钠MRI采集技术的出现,可以实现更好的分辨率和更高的SNR, 23 NaMRI得以恢复。这些研究揭示了MS大脑中病理性总钠浓度,现在甚至可以(部分)区分细胞内和细胞外钠的积累。在本篇综述中,我们(1)演示 23 NaMRI的物理基础和成像技术,以及(2)重点研究 23 NaMRI的当前和未来临床应用。因此,MS强调了其作为神经炎症和变性生物标志物的潜力。

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