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首页> 外文期刊>Journal of Cell Science >The doublecortin-related gene zyg-8 is a microtubule organizer in Caenorhabditis elegans neurons
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The doublecortin-related gene zyg-8 is a microtubule organizer in Caenorhabditis elegans neurons

机译:双击素相关的基因Zyg-8是Caenorhabdise Legans神经元的微管组织者

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摘要

Doublecortin-domain containing (DCDC) genes play key roles in the normal and pathological development of the human brain cortex. The origin of the cellular specialisation and the functional redundancy of these microtubule (MT)-associated proteins (MAPs), especially those of Doublecortin (DCX) and Doublecortin-like kinase (DCLKs) genes, is still unclear. The DCX domain has the ability to control MT architecture and bundling. However, the physiological significance of such properties is not fully understood. To address these issues, we sought post-mitotic roles for zyg-8, the sole representative of the DCX-DCLK subfamily of genes in C. elegans. Previously, zyg-8 has been shown to control anaphase-spindle positioning in one-cell stage embryos, but functions of the gene later in development have not been investigated. Here we show that wild-type zyg-8 is required beyond early embryonic divisions for proper development, spontaneous locomotion and touch sensitivity of adult worms. Consistently, we find zyg-8 expression in the six touch receptor neurons (TRNs), as well as in a subset of other neuronal and non-neuronal cells. In TRNs and motoneurons, zyg-8 controls cell body shape/polarity and process outgrowth and morphology. Ultrastructural analysis of mutant animals reveals that zyg-8 promotes structural integrity, length and number of individual MTs, as well as their bundled organisation in TRNs, with no impact on MT architecture.
机译:含有(DCDC)基因的双峰素域在人脑皮层的正常和病理发育中起关键作用。细胞专业化的起源和这些微管(MT) - 分配蛋白(MAPS),尤其是双蛋白(DCX)和双峰素样激酶(DCLEC)基因的函数冗余仍然尚不清楚。 DCX域具有控制MT架构和捆绑的能力。然而,这些性质的生理意义尚未完全理解。为了解决这些问题,我们为Zyg-8寻求了ZYG-8后的纺丝体作用,该lex-dclk亚家族的DCX-DCLK亚家族的唯一代表。以前,已显示Zyg-8控制一个细胞阶段胚胎中的后轴主轴定位,但尚未研究在发育后的基因的功能。在这里,我们表明,超越早期胚胎部门需要野生型ZYG-8,以适当的发展,自发运动和成人蠕虫的触摸敏感性。始终如一地,我们在六个触摸受体神经元(TRNS)中发现Zyg-8表达,以及其他神经元和非神经元细胞的子集。在TRNS和MOTONEURON中,ZYG-8控制细胞体形状/极性和过程的产后和形态。突变动物的超微结构分析表明,ZYG-8促进了单个MT的结构完整性,长度和数量,以及其捆绑的TRNS组织,对MT架构没有影响。

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