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表达低水平甘氨酸受体β亚基的转基因痉挛小鼠的短暂神经运动表型:惊吓疾病的动物模型

Transient neuromotor phenotype in transgenic spastic mice expressing low levels of glycine receptor beta-subunit: an animal model of startle disease.

作者信息

Becker L, Hartenstein B, Schenkel J, Kuhse J, Betz H, Weiher H

机构信息

Institut für Diabetesforschung, Kölner Platz 1, 80804 München, Germany.

出版信息

Eur J Neurosci. 2000 Jan;12(1):27-32. doi: 10.1046/j.1460-9568.2000.00877.x.

Abstract

Startle disease or hereditary hyperekplexia has been shown to result from mutations in the alpha1-subunit gene of the inhibitory glycine receptor (GlyR). In hyperekplexia patients, neuromotor symptoms generally become apparent at birth, improve with age, and often disappear in adulthood. Loss-of-function mutations of GlyR alpha or beta-subunits in mice show rather severe neuromotor phenotypes. Here, we generated mutant mice with a transient neuromotor deficiency by introducing a GlyR beta transgene into the spastic mouse (spa/spa), a recessive mutant carrying a transposon insertion within the GlyR beta-subunit gene. In spa/spa TG456 mice, one of three strains generated with this construct, which expressed very low levels of GlyR beta transgene-dependent mRNA and protein, the spastic phenotype was found to depend upon the transgene copy number. Notably, mice carrying two copies of the transgene showed an age-dependent sensitivity to tremor induction, which peaked at approximately 3-4 weeks postnatally. This closely resembles the development of symptoms in human hyperekplexia patients, where motor coordination significantly improves after adolescence. The spa/spa TG456 line thus may serve as an animal model of human startle disease.

摘要

惊吓症或遗传性易惊症已被证明是由抑制性甘氨酸受体(GlyR)的α1亚基基因突变引起的。在易惊症患者中,神经运动症状通常在出生时就很明显,随着年龄增长而改善,并且在成年后常常消失。小鼠中GlyRα或β亚基的功能丧失突变表现出相当严重的神经运动表型。在此,我们通过将GlyRβ转基因导入痉挛小鼠(spa/spa)中,产生了具有短暂神经运动缺陷的突变小鼠,痉挛小鼠是一种隐性突变体,其GlyRβ亚基基因内有一个转座子插入。在spa/spa TG456小鼠中(用该构建体产生的三个品系之一,其表达非常低水平的GlyRβ转基因依赖性mRNA和蛋白质),发现痉挛表型取决于转基因拷贝数。值得注意的是,携带两个转基因拷贝的小鼠对震颤诱导表现出年龄依赖性敏感性,在出生后约3-4周达到峰值。这与人类易惊症患者症状的发展非常相似,人类患者在青春期后运动协调性会显著改善。因此,spa/spa TG456品系可能作为人类惊吓症的动物模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c993/3655541/d82a70938449/ejn0012-0027-f1.jpg

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