果蝇的spaghetti和doubletime将生物钟和光线与半胱天冬酶、细胞凋亡及tau蛋白病联系起来。
Drosophila spaghetti and doubletime link the circadian clock and light to caspases, apoptosis and tauopathy.
作者信息
Means John C, Venkatesan Anandakrishnan, Gerdes Bryan, Fan Jin-Yuan, Bjes Edward S, Price Jeffrey L
机构信息
Division of Molecular Biology and Biochemistry, School of Biological Sciences, University of Missouri-Kansas City, Kansas City, Missouri, United States of America.
Division of Molecular Biology and Biochemistry, School of Biological Sciences, University of Missouri-Kansas City, Kansas City, Missouri, United States of America; Department of Neurology and Cognitive Neuroscience, School of Medicine, University of Missouri-Kansas City, Kansas City, Missouri, United States of America.
出版信息
PLoS Genet. 2015 May 7;11(5):e1005171. doi: 10.1371/journal.pgen.1005171. eCollection 2015 May.
While circadian dysfunction and neurodegeneration are correlated, the mechanism for this is not understood. It is not known if age-dependent circadian dysfunction leads to neurodegeneration or vice-versa, and the proteins that mediate the effect remain unidentified. Here, we show that the knock-down of a regulator (spag) of the circadian kinase Dbt in circadian cells lowers Dbt levels abnormally, lengthens circadian rhythms and causes expression of activated initiator caspase (Dronc) in the optic lobes during the middle of the day or after light pulses at night. Likewise, reduced Dbt activity lengthens circadian period and causes expression of activated Dronc, and a loss-of-function mutation in Clk also leads to expression of activated Dronc in a light-dependent manner. Genetic epistasis experiments place Dbt downstream of Spag in the pathway, and Spag-dependent reductions of Dbt are shown to require the proteasome. Importantly, activated Dronc expression due to reduced Spag or Dbt activity occurs in cells that do not express the spag RNAi or dominant negative Dbt and requires PDF neuropeptide signaling from the same neurons that support behavioral rhythms. Furthermore, reduction of Dbt or Spag activity leads to Dronc-dependent Drosophila Tau cleavage and enhanced neurodegeneration produced by human Tau in a fly eye model for tauopathy. Aging flies with lowered Dbt or Spag function show markers of cell death as well as behavioral deficits and shortened lifespans, and even old wild type flies exhibit Dbt modification and activated caspase at particular times of day. These results suggest that Dbt suppresses expression of activated Dronc to prevent Tau cleavage, and that the circadian clock defects confer sensitivity to expression of activated Dronc in response to prolonged light. They establish a link between the circadian clock factors, light, cell death pathways and Tau toxicity, potentially via dysregulation of circadian neuronal remodeling in the optic lobes.
虽然昼夜节律功能障碍与神经退行性变相关,但其机制尚不清楚。目前尚不清楚年龄依赖性昼夜节律功能障碍是否会导致神经退行性变,反之亦然,介导这种效应的蛋白质仍未确定。在这里,我们表明,在昼夜节律细胞中敲低昼夜节律激酶Dbt的调节因子(spag)会异常降低Dbt水平,延长昼夜节律,并在中午或夜间光脉冲后导致视叶中活化起始半胱天冬酶(Dronc)的表达。同样,降低Dbt活性会延长昼夜节律周期并导致活化Dronc的表达,而Clk的功能丧失突变也会以光依赖的方式导致活化Dronc的表达。遗传上位性实验表明,在该通路中Dbt位于Spag的下游,并且Spag依赖性的Dbt减少被证明需要蛋白酶体。重要的是,由于Spag或Dbt活性降低而导致的活化Dronc表达发生在不表达spag RNAi或显性负性Dbt的细胞中,并且需要来自支持行为节律的相同神经元的PDF神经肽信号传导。此外,降低Dbt或Spag活性会导致Dronc依赖性的果蝇Tau蛋白切割,并在tauopathy的果蝇眼模型中增强人Tau蛋白引起的神经退行性变。Dbt或Spag功能降低的衰老果蝇表现出细胞死亡标记以及行为缺陷和寿命缩短,甚至年老的野生型果蝇在一天中的特定时间也表现出Dbt修饰和活化的半胱天冬酶。这些结果表明,Dbt抑制活化Dronc的表达以防止Tau蛋白切割,并且昼夜节律时钟缺陷赋予对延长光照下活化Dronc表达的敏感性。它们在昼夜节律时钟因子、光、细胞死亡途径和Tau毒性之间建立了联系,可能是通过视叶中昼夜节律神经元重塑的失调。
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