Buckwalter M S, Testa C M, Noebels J L, Camper S A
Department of Human Genetics, University of Michigan Medical School, Ann Arbor 48109-0618.
Genomics. 1993 Aug;17(2):279-86. doi: 10.1006/geno.1993.1322.
Spasmodic (spd) is a recessive mouse mutation characterized by a prolonged righting reflex, fine motor tremor, leg clasping, and stiffness. Using an intersubspecific backcross that segregates spd, we placed spd on Chr 11 with the following gene order: Adra-1-3.8 +/- 2.1 cM-Pad-1-6.3 +/- 2.7-(spd, Anx-6, Csfgm, Glr-1, Il-3, Il-4, Il-5, Sparc)-9.1 +/- 2.4-D11 Mit5-2.2 +/- 1.5-Asgr-1. This localization eliminated the alpha 1-adrenergic receptor (Adra-1) and the alpha 1 and gamma 2 subunits of the GABAA receptor as candidate genes. Two other promising candidate genes, annexin VI (Anx-6) and a glutamate receptor (Glr-1), were mapped to within 2.1 cM of the spd locus. Although no recombination was observed between spd and Anx-6 or Glr-1, no evidence was obtained for a lesion in either gene. The presence of normal Anx-6 and Glr-1 mRNA transcripts was confirmed by Northern blot analysis, in situ hybridization, and DNA sequence analysis. The localization of Anx-6 and Glr-1 extends the known synteny homology between human chromosome 5q21-q31 and mouse Chr 11 and reveals the probable chromosomal location of the human counterpart to spd. Synteny homology and phenotypic similarities suggest that spasmodic mice may be a genetic model for the inherited human startle disease, hyperekplexia (STHE).
痉挛(spd)是一种隐性小鼠突变,其特征为翻正反射延长、精细运动震颤、腿部紧握和僵硬。利用分离spd的种间回交,我们将spd定位在11号染色体上,基因顺序如下:Adra-1-3.8±2.1 cM-Pad-1-6.3±2.7-(spd、Anx-6、Csfgm、Glr-1、Il-3、Il-4、Il-5、Sparc)-9.1±2.4-D11 Mit5-2.2±1.5-Asgr-1。这一定位排除了α1-肾上腺素能受体(Adra-1)以及GABAA受体的α1和γ2亚基作为候选基因。另外两个有前景的候选基因,膜联蛋白VI(Anx-6)和谷氨酸受体(Glr-1),被定位在spd基因座的2.1 cM范围内。尽管在spd与Anx-6或Glr-1之间未观察到重组,但未获得任一基因存在损伤的证据。通过Northern印迹分析、原位杂交和DNA序列分析证实了正常Anx-6和Glr-1 mRNA转录本的存在。Anx-6和Glr-1的定位扩展了人类5号染色体q21-q31与小鼠11号染色体之间已知的同线性同源性,并揭示了spd人类对应物可能的染色体位置。同线性同源性和表型相似性表明,痉挛小鼠可能是遗传性人类惊吓疾病——惊跳症(STHE)的遗传模型。
