RNA 结合蛋白功能障碍将多发性硬化症的烟熏/缓慢扩展病变与神经退行性变联系起来。

IF 8.1 1区 医学 Q1 CLINICAL NEUROLOGY Annals of Neurology Pub Date : 2024-10-18 DOI:10.1002/ana.27114
Miranda L Messmer, Hannah E Salapa, Bogdan F Popescu, Michael C Levin
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引用次数: 0

摘要

目的:尽管多发性硬化症(MS)的治疗方法不断进步,但持续的神经变性仍在导致残疾和疾病进展。燃烧/缓慢扩展病变(SELs)和 RNA 结合蛋白(RBP)异质核糖核蛋白 A1(hnRNP A1)功能障碍是多发性硬化症皮质的病理特征,分别与残疾和神经变性密切相关。我们假设神经元 hnRNP A1 功能障碍会导致神经变性,并因进行性多发性硬化症中的烟熏/SELs 而加剧:方法:使用免疫组化方法检测健康对照组和多发性硬化症患者大脑中神经元 hnRNP A1 的病理变化(hnRNP A1 的核胞质错定位)。根据 hnRNP A1 病理学的严重程度对多发性硬化症病例进行分层,以研究 RBP 功能障碍、脱髓鞘和神经变性之间的联系:结果:我们发现,烟雾状/SELs仅存在于以邻近皮质灰质中神经元hnRNP A1病理学升高(MS-A1高)为特征的MS组织亚群中。与健康对照组和 hnRNP A1 病理变化较低的 MS(MS-A1-low)相比,MS-A1high 显示出神经变性标志物的升高,包括神经元丢失和损伤、脑萎缩、轴突丢失和轴突变性。此外,我们还在 MS-A1high 病例的皮质投射神经元中发现了一个形态完整的神经元亚群,该亚群缺乏神经元特异性 RBP NeuN 的表达。NeuN阴性神经元的发现表明,一些皮质神经元可能只是受伤而不是丧失。通过描述多发性硬化症皮质中 RBP 的病理特征,这项研究对了解驱动神经变性的致病机制、残疾和疾病进展的基质具有重要意义。ann neurol 2024.
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RNA Binding Protein Dysfunction Links Smoldering/Slowly Expanding Lesions to Neurodegeneration in Multiple Sclerosis.

Objective: Despite the advances in treatments for multiple sclerosis (MS), unremitting neurodegeneration continues to drive disability and disease progression. Smoldering/slowly expanding lesions (SELs) and dysfunction of the RNA binding protein (RBP) heterogeneous nuclear ribonucleoprotein A1 (hnRNP A1) are pathologic hallmarks of MS cortex and intricately tied to disability and neurodegeneration, respectively. We hypothesized that neuronal hnRNP A1 dysfunction contributes to neurodegeneration and is exacerbated by smoldering/SELs in progressive MS.

Methods: Neuronal hnRNP A1 pathology (nucleocytoplasmic mislocalization of hnRNP A1) was examined in healthy control and MS brains using immunohistochemistry. MS cases were stratified by severity of hnRNP A1 pathology to examine the link between RBP dysfunction, demyelination, and neurodegeneration.

Results: We found that smoldering/SELs were only present within a subset of MS tissues characterized by elevated neuronal hnRNP A1 pathology (MS-A1high) in adjacent cortical gray matter. In contrast to healthy controls and MS with low hnRNP A1 pathology (MS-A1low), MS-A1high showed elevated markers of neurodegeneration, including neuronal loss and injury, brain atrophy, axonal loss, and axon degeneration. Additionally, we discovered a subpopulation of morphologically intact neurons lacking expression of NeuN, a neuron-specific RBP, in cortical projection neurons in MS-A1high cases.

Interpretation: hnRNP A1 dysfunction contributes to neurodegeneration and may be exacerbated by smoldering/SELs in progressive MS. The discovery of NeuN-negative neurons suggests that some cortical neurons may only be injured and not lost. By characterizing RBP pathology in MS cortex, this study has important implications for understanding the pathogenic mechanisms driving neurodegeneration, the substrate of disability and disease progression. ANN NEUROL 2024.

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来源期刊
Annals of Neurology
Annals of Neurology 医学-临床神经学
CiteScore
18.00
自引率
1.80%
发文量
270
审稿时长
3-8 weeks
期刊介绍: Annals of Neurology publishes original articles with potential for high impact in understanding the pathogenesis, clinical and laboratory features, diagnosis, treatment, outcomes and science underlying diseases of the human nervous system. Articles should ideally be of broad interest to the academic neurological community rather than solely to subspecialists in a particular field. Studies involving experimental model system, including those in cell and organ cultures and animals, of direct translational relevance to the understanding of neurological disease are also encouraged.
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