首页> 外文期刊>Neuroscience Letters: An International Multidisciplinary Journal Devoted to the Rapid Publication of Basic Research in the Brain Sciences >The kinesin light chain gene: its mapping and exclusion in mouse and human forms of inherited motor neuron degeneration.
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The kinesin light chain gene: its mapping and exclusion in mouse and human forms of inherited motor neuron degeneration.

机译:驱动蛋白轻链基因:其在小鼠​​和人类形式的遗传性运动神经元变性中的定位和排除。

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摘要

The underlying genetic cause is known for only 10-20% of familial motor neuron disease (MND). Thus the genes involved in the aetiology of 80-90% of familial MND remain to be determined, and animal models are powerful tools for undertaking this task. We have mapped a heritable form of motor neuron degeneration in the mouse to a region that has homology to human chromosome 14q32.1-qter. This region contains the kinesin light chain gene (KLC1), which is a candidate for involvement in motor neuron degeneration because of its function in the motor-protein kinesin, and its neuronal expression. To investigate the role of KLC1 in a mouse motor neuron degeneration mutant that we are studying, we have identified mouse Klc1 gene sequences and mapped them with respect to our mutant locus. We have also investigated KLC1 in human patients with familial MND. Based on recombination and the absence of mutations in the coding region of KLC1, this gene can be excluded as a candidate gene in our mouse mutation and, where we have investigated, it is normal in human familial MND.
机译:潜在的遗传原因仅占家族运动神经元疾病(MND)的10-20%。因此,涉及80-90%家族性MND病因的基因尚待确定,而动物模型是完成此任务的有力工具。我们已经在小鼠中将可遗传形式的运动神经元变性映射到与人类染色体14q32.1-qter具有同源性的区域。该区域包含驱动蛋白轻链基因(KLC1),由于其在运动蛋白驱动蛋白中的功能及其神经元表达,因此是参与运动神经元变性的候选基因。若要调查KLC1在我们正在研究的小鼠运动神经元变性突变体中的作用,我们已经鉴定了小鼠Klc1基因序列,并根据我们的突变体基因座对其进行了定位。我们还研究了家族性MND患者的KLC1。基于重组和KLC1编码区中不存在突变,该基因可以作为我们小鼠突变中的候选基因而排除,并且在我们研究的地方,它在人家族性MND中是正常的。

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