Axonal degeneration is a major determinant of permanent neurological impairment during multiple sclerosis (MS). Due to the variable course of clinical disease and the heterogeneity of MS lesions, the mechanisms governing axonal degeneration may differ between disease stages. While the etiology of MS remains elusive, there now exist potential prognostic biomarkers that can predict the conversion to clinically definite MS. Specialized imaging techniques identifying axonal injury and drop-out are becoming established in clinical practice as a predictive measure of MS progression, such as optical coherence tomography (OCT) or diffusion tensor imaging (DTI). However, these imaging techniques are still being debated as predictive biomarkers since controversy surrounds their lesion-specific association with expanded disability status scale (EDSS). A more promising diagnostic measure of axonal degeneration has been argued for the detection of reduced N-acetyl aspartate (NAA) and Creatine ratios via magnetic resonance spectroscopic (MRS) imaging, but again fail with its specificity for predicting actual axonal degeneration. Greater accuracy of predictive biomarkers is therefore warranted and may include CSF neurofilament light chain (NF-L) and neurofilament heavy chain (NF-H) levels, for progressive MS. Furthermore, defining the molecular mechanisms that occur during the neurodegenerative changes in the various subgroups of MS may in fact prove vital for the future development of efficacious neuroprotective therapies. The clinical translation of a combined Na+ and Ca2+ channel blocker may lead to the establishment of a bona fide neuroprotective agent for the treatment of progressive MS. However, more specific therapeutic targets to limit axonal damage in MS need investigation and may include such integral axonal proteins such as the collapsin response mediator protein-2 (CRMP-2), a molecule which upon post-translational modification may propagate axonal degeneration in MS. In this review, we discuss the current clinical determinants of axonal damage in MS and consider the cellular and molecular mechanisms that may initiate these neurodegenerative changes. In particular we highlight the therapeutic candidates that may formulate novel therapeutic strategies to limit axonal degeneration and EDSS during progressive MS.
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机译:轴突变性是多发性硬化症(MS)期间永久性神经功能缺损的主要决定因素。由于临床疾病的变化过程和MS病变的异质性,控制轴突变性的机制在疾病阶段之间可能有所不同。虽然MS的病因仍然难以捉摸,但现在存在潜在的预后生物标志物,可以预测其向临床确定的MS的转化。识别轴突损伤和脱落的专门成像技术已在临床实践中确立,作为MS进展的预测指标,例如光学相干断层扫描(OCT)或弥散张量成像(DTI)。但是,这些成像技术仍被作为预测性生物标志物进行辩论,因为争议围绕着它们的病变特异性关联与扩大的残疾状态量表(EDSS)。对于通过磁共振波谱(MRS)成像检测降低的N-乙酰天门冬氨酸(NAA)和肌酸比率,已经提出了一种更有希望的轴突变性诊断方法,但是它仍然无法预测轴突变性。因此,预测性生物标志物的准确性更高,而且对于进行性MS可能包括CSF神经丝轻链(NF-L)和神经丝重链(NF-H)水平。此外,确定在MS的各个亚组中神经退行性变化期间发生的分子机制实际上可能被证明对于有效的神经保护疗法的未来发展至关重要。 Na + 和Ca 2 + 联合通道阻滞剂的临床翻译可能会导致建立真正的神经保护剂来治疗进行性MS。但是,需要进一步研究以限制MS中轴突损伤的更具体的治疗靶标,并且可能包括此类完整的轴突蛋白,例如collapsin反应介质蛋白2(CRMP-2),这种分子在翻译后修饰后可在MS中传播轴突变性。在这篇综述中,我们讨论了MS中轴突损伤的当前临床决定因素,并考虑了可能引发这些神经退行性改变的细胞和分子机制。特别是,我们重点介绍了可以制定新的治疗策略以限制进行性MS期间轴突变性和EDSS的治疗候选药物。
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