首页> 美国卫生研究院文献>The Journal of Neuroscience >The Drosophila Receptor Protein Tyrosine Phosphatase LAR Is Required for Development of Circadian Pacemaker Neuron Processes That Support Rhythmic Activity in Constant Darkness But Not during Light/Dark Cycles
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The Drosophila Receptor Protein Tyrosine Phosphatase LAR Is Required for Development of Circadian Pacemaker Neuron Processes That Support Rhythmic Activity in Constant Darkness But Not during Light/Dark Cycles

机译:果蝇起搏器神经元过程的发展需要果蝇受体蛋白酪氨酸磷酸酶LAR该过程支持恒定黑暗中的节律活动但在明/暗周期中不支持

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摘要

In Drosophila, a transcriptional feedback loop that is activated by CLOCK-CYCLE (CLK-CYC) complexes and repressed by PERIOD-TIMELESS (PER-TIM) complexes keeps circadian time. The timing of CLK-CYC activation and PER-TIM repression is regulated post-translationally, in part through rhythmic phosphorylation of CLK, PER, and TIM. Although kinases that control PER, TIM, and CLK levels, activity, and/or subcellular localization have been identified, less is known about phosphatases that control clock protein dephosphorylation. To identify clock-relevant phosphatases, clock-cell-specific RNAi knockdowns of Drosophila phosphatases were screened for altered activity rhythms. One phosphatase that was identified, the receptor protein tyrosine phosphatase leukocyte-antigen-related (LAR), abolished activity rhythms in constant darkness (DD) without disrupting the timekeeping mechanism in brain pacemaker neurons. However, expression of the neuropeptide pigment-dispersing factor (PDF), which mediates pacemaker neuron synchrony and output, is eliminated in the dorsal projections from small ventral lateral (sLNv) pacemaker neurons when Lar expression is knocked down during development, but not in adults. Loss of Lar function eliminates sLNv dorsal projections, but PDF expression persists in sLNv and large ventral lateral neuron cell bodies and their remaining projections. In contrast to the defects in lights-on and lights-off anticipatory activity seen in flies that lack PDF, Lar RNAi knockdown flies anticipate the lights-on and lights-off transition normally. Our results demonstrate that Lar is required for sLNv dorsal projection development and suggest that PDF expression in LNv cell bodies and their remaining projections mediate anticipation of the lights-on and lights-off transitions during a light/dark cycle.>SIGNIFICANCE STATEMENT In animals, circadian clocks drive daily rhythms in physiology, metabolism, and behavior via transcriptional feedback loops. Because key circadian transcriptional activators and repressors are regulated by phosphorylation, we screened for phosphatases that alter activity rhythms when their expression was reduced. One such phosphatase, leukocyte-antigen-related (LAR), abolishes activity rhythms, but does not disrupt feedback loop function. Rather, Lar disrupts clock output by eliminating axonal processes from clock neurons that release pigment-dispersing factor (PDF) neuropeptide into the dorsal brain, but PDF expression persists in their cell bodies and remaining projections. In contrast to flies that lack PDF, flies that lack Lar anticipate lights-on and lights-off transitions normally, which suggests that the remaining PDF expression mediates activity during light/dark cycles.
机译:在果蝇中,由CLOCK-CYCLE(CLK-CYC)复合物激活并由PERIOD-TIMELESS(PER-TIM)复合物抑制的转录反馈环保持昼夜时间。 CLK-CYC激活和PER-TIM抑制的时间在翻译后进行调节,部分通过CLK,PER和TIM的有节奏的磷酸化来调节。尽管已经确定了控制PER,TIM和CLK水平,活性和/或亚细胞定位的激酶,但对于控制时钟蛋白去磷酸化的磷酸酶知之甚少。为了鉴定与时钟相关的磷酸酶,对果蝇磷酸酶的时钟细胞特异性RNAi敲低进行了筛查,以发现活动节律的改变。鉴定出的一种磷酸酶受体蛋白酪氨酸磷酸酶白细胞抗原相关(LAR)消除了恒定黑暗(DD)中的活动节律,而没有破坏脑起搏器神经元的计时机制。但是,当发育过程中Lar表达被敲低时,介导起搏器神经元同步和输出的神经肽色素分散因子(PDF)的表达在小腹外侧(sLNv)起搏器神经元的背侧投射中被消除,而在成年人中则没有。 Lar功能的丧失消除了sLNv的背侧投射,但PDF表达在sLNv和大型腹侧神经元细胞体及其剩余的投射中仍然存在。与缺乏PDF的果蝇在开灯和熄灯预期活动中的缺陷形成对比,Lar RNAi组合果蝇可以正常预测开灯和熄灯过渡。我们的结果表明Lar是sLNv背向投射发育所必需的,并暗示LNv细胞体中的PDF表达及其剩余投射可介导在明/暗循环中对亮-灭过渡的预期。>意义声明< / strong>在动物中,生物钟通过转录反馈回路驱动生理,代谢和行为的日常节律。由于关键的昼夜节律转录激活因子和阻遏因子受磷酸化作用的调节,因此我们筛选了磷酸酶,这些磷酸酶可在其表达减少时改变活动节奏。一种这样的磷酸酶,白细胞抗原相关(LAR),可消除活动节律,但不会破坏反馈回路功能。相反,Lar通过消除时钟神经元的轴突过程来破坏时钟输出,该时钟神经元将色素分散因子(PDF)神经肽释放到背脑中,但PDF表达仍在其细胞体内和其余的投射区域内。与缺少PDF的果蝇相反,缺少Lar的果蝇通常会正常地进行亮灯和灭灯的转换,这表明剩余的PDF表达会在明/暗周期中介导活性。

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