绵羊CLN5和CLN6神经元样脂褐变(巴滕病)的神经病理学特征

IF 2.7 4区 医学 Q2 DEVELOPMENTAL BIOLOGY
Nadia L. Mitchell, Katharina N. Russell, Graham K. Barrell, Imke Tammen, David N. Palmer
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引用次数: 3

摘要

绵羊患有自然发生的CLN5和CLN6形式的神经性ceroid脂褐病(Batten病),具有人类疾病的关键临床特征,是开发和测试基因治疗临床疗效的理想模型系统。然而,首先重要的是表征受影响羊的疾病进展所发生的神经病理变化。本研究比较了从出生到≤24月龄终末期疾病,Borderdale羊CLN5、South Hampshire羊CLN6和美利奴羊大脑中神经退行性变、神经炎症和溶酶体蓄积。尽管基因产物、突变和亚细胞定位非常不同,但三种疾病模型的致病级联反应非常相似。受影响的绵羊在出生时就存在神经胶质激活,并先于神经元丧失,从视觉和顶枕皮质(与临床症状最显著相关)扩散到终末期疾病的整个皮质套。相比之下,皮层下区域较少受累,但随着年龄的增长,溶酶体储存量在患病羊的大脑中呈近线性增长。这些神经病理变化与已发表的临床数据的相关性确定了受影响羊的三个潜在治疗窗口期——症状前(3个月)、症状早期(6个月)和症状疾病后期(9个月)——超过这三个阶段,神经元的广泛消耗可能会减少任何治疗益处的机会。绵羊CLN5和CLN6疾病的神经病理变化的综合自然史将是确定治疗在每个疾病阶段的影响的组成部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Characterization of neuropathology in ovine CLN5 and CLN6 neuronal ceroid lipofuscinoses (Batten disease)

Characterization of neuropathology in ovine CLN5 and CLN6 neuronal ceroid lipofuscinoses (Batten disease)

Sheep with naturally occurring CLN5 and CLN6 forms of neuronal ceroid lipofuscinoses (Batten disease) share the key clinical features of the human disease and represent an ideal model system in which the clinical efficacy of gene therapies is developed and test. However, it was first important to characterize the neuropathological changes that occur with disease progression in affected sheep. This study compared neurodegeneration, neuroinflammation, and lysosomal storage accumulation in CLN5 affected Borderdale, CLN6 affected South Hampshire, and Merino sheep brains from birth to end-stage disease at ≤24 months of age. Despite very different gene products, mutations, and subcellular localizations, the pathogenic cascade was remarkably similar for all three disease models. Glial activation was present at birth in affected sheep and preceded neuronal loss, with both spreading from the visual and parieto-occipital cortices most prominently associated with clinical symptoms to the entire cortical mantle by end-stage disease. In contrast, the subcortical regions were less involved, yet lysosomal storage followed a near-linear increase across the diseased sheep brain with age. Correlation of these neuropathological changes with published clinical data identified three potential therapeutic windows in affected sheep—presymptomatic (3 months), early symptomatic (6 months), and a later symptomatic disease stage (9 months of age)—beyond which the extensive depletion of neurons was likely to diminish any chance of therapeutic benefit. This comprehensive natural history of the neuropathological changes in ovine CLN5 and CLN6 disease will be integral in determining what impact treatment has at each of these disease stages.

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来源期刊
Developmental Neurobiology
Developmental Neurobiology 生物-发育生物学
CiteScore
6.50
自引率
0.00%
发文量
45
审稿时长
4-8 weeks
期刊介绍: Developmental Neurobiology (previously the Journal of Neurobiology ) publishes original research articles on development, regeneration, repair and plasticity of the nervous system and on the ontogeny of behavior. High quality contributions in these areas are solicited, with an emphasis on experimental as opposed to purely descriptive work. The Journal also will consider manuscripts reporting novel approaches and techniques for the study of the development of the nervous system as well as occasional special issues on topics of significant current interest. We welcome suggestions on possible topics from our readers.
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