Circular breakdown of neural networks due to loss of deubiquitinating enzyme (UCH-L1) in gracile axonal dystrophy (gad) mouse

IF 0.7 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY
T. Kikuchi
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Abstract

Gracile axonal dystrophy (gad) mouse shows tremor, ataxia and muscular atrophy of hind limbs from about 80-days of age. These clinical features become progressively severe to death. Pathological examination reveals that main and early axonal degeneration exists in a long ascending nervous tract in dorsal column of the spinal cord: gracile nucleus and fascicules. Similar lesions are seen in axonal terminals of peripheral sensory (muscle spindles) and motor endplates. Most striking features of axonal dystrophy are “dying-back” axonal degeneration with partial swellings (“spheroids” in matured type) which come to be most frequently in gracile nucleus, followed by in order of gracile fasciculus of cervical, thoracic and lumber cord levels. Immunocytochemical increase of glial fibrillary acidic protein (GFAP) and substance P (SP) is seen in reactive astrocytes and degenerating axons. Likewise, amyloid precursor protein (APP) and amyloid β-protein (AβP) activity become positive in axons and astrocytes along ascending tract. Moreover, ubiquitin-positive dot-like structures accumulate in gracile nucleus, spinocerebellar tract, and cerebellum in gad mice after 9th-week old. Ubiquitinated structures are localized in spheroids with a larger diameter than normal. The gad mutation is caused by an in-frame deletion including exon 7 and 8 of UCH-L1 gene, encoding the ubiquitin c-terminal hydrolase (UCH) isozyme (UCH-L1) selectively expressed in nervous system and testis/ovary. The gad allele encodes a truncated UCH-L1 lacking a segment of 42 amino acids containing catalytic site. The evaluation as mouse models for Parkinson's and Alzheimer's diseases and the collapse of synapse-axon circulation around central nervous system from peripheral nervous system are discussed.
细轴突营养不良(gad)小鼠中去泛素化酶(UCH-L1)缺失导致的神经网络循环破坏
细轴突营养不良小鼠从80日龄开始出现震颤、共济失调和后肢肌肉萎缩。这些临床特征逐渐严重到死亡。病理检查显示脊髓背柱的长上行神经束:细核和神经束存在主要的和早期的轴突变性。外周感觉神经(肌梭)和运动终板的轴突终末也可见类似病变。轴突营养不良最显著的特征是轴突退行性变伴部分肿胀(成熟型为球状),最常见于细核,其次为颈、胸、脊髓细束。在反应性星形胶质细胞和变性轴突中可见胶质原纤维酸性蛋白(GFAP)和P物质(SP)的免疫细胞化学增加。同样,淀粉样前体蛋白(APP)和淀粉样β蛋白(AβP)活性在上行束轴突和星形胶质细胞中呈阳性。此外,9周龄后,泛素阳性的点状结构在小鼠的细核、脊髓小脑束和小脑中积累。泛素化结构位于比正常直径大的球体中。该基因突变是由编码泛素c端水解酶(UCH- l1)同工酶(UCH- l1)在神经系统和睾丸/卵巢选择性表达的UCH- l1基因的7和8外显子框内缺失引起的。gad等位基因编码一个截断的UCH-L1,缺少含有催化位点的42个氨基酸片段。本文讨论了作为帕金森病和阿尔茨海默病小鼠模型的评价以及周围神经系统突触-轴突循环的崩溃。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
AIMS Molecular Science
AIMS Molecular Science BIOCHEMISTRY & MOLECULAR BIOLOGY-
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审稿时长
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