Lee SeoJin, Panthi Sandesh, Jo Hyun Woo, Cho Jaeyoung, Kim Min-Sik, Jeong Na Young, Song In Ok, Jung Junyang, Huh Youngbuhm
Department of Biomedical Science, Graduate School, Kyung Hee University, Dongdaemun-gu, Seoul, Korea.
Department of Medicine, Graduate School, Kyung Hee University, Dongdaemun-gu, Seoul, Korea.
Neural Regen Res. 2017 Mar;12(3):486-492. doi: 10.4103/1673-5374.202920.
Dominant intermediate Charcot-Marie-Tooth disease type C (DI-CMTC) is a dominantly inherited neuropathy that has been classified primarily based on motor conduction velocity tests but is now known to involve axonal and demyelination features. DI-CMTC is linked to tyrosyl-tRNA synthetase (YARS)-associated neuropathies, which are caused by E196K and G41R missense mutations and a single deletion (153-156delVKQV). It is well-established that these YARS mutations induce neuronal dysfunction, morphological symptoms involving axonal degeneration, and impaired motor performance. The present study is the first to describe a novel mouse model of YARS-mutation-induced neuropathy involving a neuron-specific promoter with a deleted mitochondrial targeting sequence that inhibits the expression of YARS protein in the mitochondria. An adenovirus vector system and techniques were utilized to express YARS fusion proteins with a Flag-tag in the spinal cord, peripheral axons, and dorsal root ganglia. Following transfection of YARS-expressing viruses, the distributions of wild-type (WT) YARS and E196K mutant proteins were compared in all expressed regions; G41R was not expressed. The proportion of Flag/green fluorescent protein (GFP) double-positive signaling in the E196K mutant-type mice did not significantly differ from that of WT mice in dorsal root ganglion neurons. All adenovirus genes, and even the empty vector without the YARS gene, exhibited GFP-positive signaling in the ventral horn of the spinal cord because GFP in an adenovirus vector is driven by a cytomegalovirus promoter. The present study demonstrated that anatomical differences in tissue can lead to dissimilar expressions of YARS genes. Thus, use of this novel animal model will provide data regarding distributional defects between mutant and WT genes in neurons, the DI-CMTC phenotype, and potential treatment approaches for this disease.
显性中间型C型遗传性运动感觉神经病(DI-CMTC)是一种常染色体显性遗传性神经病变,最初主要根据运动神经传导速度测试进行分类,但现在已知其涉及轴突和脱髓鞘特征。DI-CMTC与酪氨酰-tRNA合成酶(YARS)相关的神经病变有关,后者由E196K和G41R错义突变以及一个单一缺失(153-156delVKQV)引起。众所周知,这些YARS突变会导致神经元功能障碍、涉及轴突变性的形态学症状以及运动能力受损。本研究首次描述了一种新型的YARS突变诱导的神经病变小鼠模型,该模型涉及一个神经元特异性启动子,其线粒体靶向序列缺失,可抑制线粒体中YARS蛋白的表达。利用腺病毒载体系统和技术在脊髓、外周轴突和背根神经节中表达带有Flag标签的YARS融合蛋白。在转染表达YARS的病毒后,比较了野生型(WT)YARS和E196K突变蛋白在所有表达区域的分布;未表达G41R。在背根神经节神经元中,E196K突变型小鼠中Flag/绿色荧光蛋白(GFP)双阳性信号的比例与WT小鼠没有显著差异。所有腺病毒基因,甚至没有YARS基因的空载体,在脊髓腹角均表现出GFP阳性信号,因为腺病毒载体中的GFP由巨细胞病毒启动子驱动。本研究表明,组织中的解剖差异可导致YARS基因表达不同。因此,使用这种新型动物模型将提供有关神经元中突变基因和WT基因之间分布缺陷、DI-CMTC表型以及该疾病潜在治疗方法的数据。
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