SMN1型
脊髓性肌萎缩
形状记忆合金*
生物
运动神经元
转基因小鼠
外显子
转基因
表型
病态的
病理
神经科学
脊髓
基因
遗传学
医学
数学
组合数学
作者
Hsiu Mei Hsieh‐Li,Jan‐Gowth Chang,Yuh‐Jyh Jong,Mei-Hsiang Wu,Nancy M. Wang,Chang Hai Tsai,Hung Li
出处
期刊:Nature Genetics
[Springer Nature]
日期:2000-01-01
卷期号:24 (1): 66-70
被引量:676
摘要
The survival motor neuron gene is present in humans in a telomeric copy, SMN1, and several centromeric copies, SMN2. Homozygous mutation of SMN1 is associated with proximal spinal muscular atrophy (SMA), a severe motor neuron disease characterized by early childhood onset of progressive muscle weakness. To understand the functional role of SMN1 in SMA, we produced mouse lines deficient for mouse Smn and transgenic mouse lines that expressed human SMN2. Smn-/- mice died during the peri-implantation stage. In contrast, transgenic mice harbouring SMN2 in the Smn-/- background showed pathological changes in the spinal cord and skeletal muscles similar to those of SMA patients. The severity of the pathological changes in these mice correlated with the amount of SMN protein that contained the region encoded by exon 7. Our results demonstrate that SMN2 can partially compensate for lack of SMN1. The variable phenotypes of Smn-/-SMN2 mice reflect those seen in SMA patients, providing a mouse model for this disease.
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