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LAS24/KOG1是雷帕霉素靶蛋白复合物1(TORC1)的一个组成部分,在酵母中对局部麻醉药丁卡因的抗性及肌动蛋白细胞骨架的正常分布是必需的。

LAS24/KOG1, a component of the TOR complex 1 (TORC1), is needed for resistance to local anesthetic tetracaine and normal distribution of actin cytoskeleton in yeast.

作者信息

Araki Tomoyuki, Uesono Yukifumi, Oguchi Tomoko, Toh-E Akio

机构信息

Department of Biological Science, Graduate School of Science, University of Tokyo, Hongo, Japan.

出版信息

Genes Genet Syst. 2005 Oct;80(5):325-43. doi: 10.1266/ggs.80.325.

Abstract

It is known that some local anesthetics inhibit the growth of budding yeast cells. To investigate the pathway of local anesthetics' action, we isolated and characterized mutants that were hyper-sensitive to tetracaine, and at the same time, temperature-sensitive for growth. They were collectively called las (local anesthetic sensitive) mutants. One of the LAS genes, LAS24, was found to be identical to KOG1, which had been independently discovered as a member of the TOR complex 1 (TORC1). Las24p/Kog1p is a widely conserved TOR binding protein containing the NRC domain, HEAT repeats and WD-40 repeats, but its function remains unknown. Like the tor mutants, the las24 mutants were found to have a defect in cell wall integrity and to show sensitivity to rapamycin. Furthermore, Las24p is required not only in TORC1-mediated (rapamycin-sensitive) pathways such as translation initiation control and phosphorylation of Npr1p and Gln3p, but also for the normal distribution of the actin cytoskeleton, which has been regarded as a TORC2-mediated event. Intriguingly, the temperature-sensitivity of the las24 mutant was suppressed by either activation of Tap42/PPase or by down-regulation of the RAS/cAMP pathway. Suppressors of the temperature-sensitivity of the las24-1 mutant were found not to be effective for suppression of the tetracaine-sensitivity of the same mutant. These observations along with the facts that tetracaine and high temperature differentially affected the las24-1 mutant suggest that Las24p/Kog1p is not a target of tetracaine and that the tetracaine-sensitive step may be one of downstream branches of the TORC1 pathway. Consistent with the broad cellular functions exerted by the TOR pathway, we found that Las24p was associated with membranes and was localized at vacuoles, the plasma membrane and small vesicles.

摘要

已知一些局部麻醉剂会抑制出芽酵母细胞的生长。为了研究局部麻醉剂的作用途径,我们分离并鉴定了对丁卡因高度敏感且对生长温度敏感的突变体。它们被统称为las(局部麻醉剂敏感)突变体。其中一个LAS基因LAS24被发现与KOG1相同,KOG1此前已被独立鉴定为雷帕霉素靶蛋白复合体1(TORC1)的成员之一。Las24p/Kog1p是一种广泛保守的TOR结合蛋白,包含NRC结构域、HEAT重复序列和WD-40重复序列,但其功能仍不清楚。与tor突变体一样,las24突变体被发现存在细胞壁完整性缺陷,并对雷帕霉素敏感。此外,Las24p不仅在TORC1介导的(对雷帕霉素敏感的)途径中发挥作用,如翻译起始控制以及Npr1p和Gln3p的磷酸化,而且对于肌动蛋白细胞骨架的正常分布也是必需的,而肌动蛋白细胞骨架的正常分布一直被认为是TORC2介导的事件。有趣的是,las24突变体的温度敏感性可通过激活Tap42/PPase或下调RAS/cAMP途径来抑制。las24-1突变体温度敏感性的抑制子对该突变体丁卡因敏感性的抑制无效。这些观察结果以及丁卡因和高温对las24-1突变体产生不同影响的事实表明,Las24p/Kog1p不是丁卡因的作用靶点,且丁卡因敏感步骤可能是TORC1途径的下游分支之一。与TOR途径发挥的广泛细胞功能一致,我们发现Las24p与膜相关,并定位于液泡、质膜和小泡。

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