Robertson A M, Perea J, McGuigan A, King R H M, Muddle J R, Gabreëls-Festen A A, Thomas P K, Huxley C
Division of Biomedical Sciences, and Clinical Sciences Centre, Imperial College School of Science, Technology and Medicine, London, UK.
J Anat. 2002 Apr;200(4):377-90. doi: 10.1046/j.1469-7580.2002.00039.x.
Charcot-Marie-Tooth disease type 1A is a dominantly inherited demyelinating disorder of the peripheral nervous system. It is most frequently caused by overexpression of peripheral myelin protein 22 (PMP22), but is also caused by point mutations in the PMP22 gene. We describe a new transgenic mouse model (My41) carrying the mouse, rather than the human, pmp22 gene. The My41 strain has a severe phenotype consisting of unstable gait and weakness of the hind limbs that becomes obvious during the first 3 weeks of life. My41 mice have a shortened life span and breed poorly. Pathologically, My41 mice have a demyelinating peripheral neuropathy in which 75% of axons do not have a measurable amount of myelin. We compare the peripheral nerve pathology seen in My41 mice, which carry the mouse pmp22 gene, with previously described transgenic mice over-expressing the human PMP22 protein and Trembler-J (TrJ) mice which have a P16L substitution. We also look at the differences between CMT1A duplication patients, patients with the P16L mutation and their appropriate mouse models.
1A型夏科-马里-图斯病是一种常染色体显性遗传性周围神经系统脱髓鞘疾病。其最常见的病因是外周髓鞘蛋白22(PMP22)过度表达,但也可由PMP22基因的点突变引起。我们描述了一种携带小鼠而非人类pmp22基因的新型转基因小鼠模型(My41)。My41品系具有严重的表型,包括步态不稳和后肢无力,在出生后的前3周内变得明显。My41小鼠寿命缩短且繁殖能力差。病理上,My41小鼠患有脱髓鞘性周围神经病,其中75%的轴突没有可测量的髓鞘量。我们将携带小鼠pmp22基因的My41小鼠的周围神经病理与先前描述的过表达人类PMP22蛋白的转基因小鼠以及具有P16L替代的震颤-J(TrJ)小鼠进行比较。我们还研究了1A型遗传性运动感觉神经病(CMT1A)重复患者、P16L突变患者及其相应小鼠模型之间的差异。
