三磷酸异构体酶缺乏与黑胃果蝇突触囊泡循环失调有关。

IF 2.8 4区 医学 Q2 NEUROSCIENCES
Aelfwin Stone, Oliver Cujic, Angel Rowlett, Sophia Aderhold, Emma Savage, Bruce Graham, Joern R Steinert
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引用次数: 1

摘要

导读:许多神经退行性疾病与氧化还原应激增加引起的神经元功能障碍有关,通常与氧化还原活性分子如一氧化氮(NO)或氧自由基的异常产生有关。受氧化还原介导的变化影响的一种蛋白质是糖酵解酶三磷酸异构酶(TPI),它已被证明经历3-硝基酪氨酸化(一种no介导的翻译后修饰)使其失去活性。这种修饰所导致的神经元变化还没有得到很好的理解。然而,相关的糖基化诱导的细胞毒性已被报道,因此可能通过损害突触囊泡循环而引起神经元和突触功能障碍。方法:本研究利用黑腹果蝇(Drosophila melanogaster)来确定TPI活性改变对神经元生理的影响,将异常的TPI功能和氧化还原应激与神经元缺陷联系起来。我们使用表达TPI蛋白错义等位基因M81T的果蝇突变体,该基因在之前的筛选中被鉴定出来,并导致TPI蛋白的失活突变(TPIM81T, wstd1)。我们评估了谷氨酸能果蝇神经肌肉接点(NMJ)的突触生理学、突触形态和行为表型,以及对寿命的影响。结果:诱发和自发兴奋性连接电流的电生理记录,以及高频训练刺激和恢复方案,用于研究突触耗竭和随后的恢复。存在wstd1突变时,单突触电流没有改变,但自发事件的频率降低了。Wstd1幼虫在高频率刺激下也表现出囊泡耗竭率的增强,随后诱发的突触反应的恢复时间延长。计算模型表明,TPI突变体幼虫的活性依赖囊泡循环明显下降,表现为易释放囊泡池的恢复时间增加。NMJs的共聚焦图像显示野生型和wstd1之间没有形态学或发育差异,但TPI突变体通过嗅觉联想学习试验评估显示出学习障碍。讨论:我们的数据表明,wstd1表型部分是由于囊泡动力学的改变,包括囊泡池补充的减少和内/胞吐过程的改变。这可能导致学习和记忆障碍以及神经元功能障碍,也可能是其他已报道的神经元表型的促成因素。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Triose-phosphate isomerase deficiency is associated with a dysregulation of synaptic vesicle recycling in <i>Drosophila melanogaster</i>.

Triose-phosphate isomerase deficiency is associated with a dysregulation of synaptic vesicle recycling in <i>Drosophila melanogaster</i>.

Triose-phosphate isomerase deficiency is associated with a dysregulation of synaptic vesicle recycling in <i>Drosophila melanogaster</i>.

Triose-phosphate isomerase deficiency is associated with a dysregulation of synaptic vesicle recycling in Drosophila melanogaster.

Introduction: Numerous neurodegenerative diseases are associated with neuronal dysfunction caused by increased redox stress, often linked to aberrant production of redox-active molecules such as nitric oxide (NO) or oxygen free radicals. One such protein affected by redox-mediated changes is the glycolytic enzyme triose-phosphate isomerase (TPI), which has been shown to undergo 3-nitrotyrosination (a NO-mediated post-translational modification) rendering it inactive. The resulting neuronal changes caused by this modification are not well understood. However, associated glycation-induced cytotoxicity has been reported, thus potentially causing neuronal and synaptic dysfunction via compromising synaptic vesicle recycling.

Methods: This work uses Drosophila melanogaster to identify the impacts of altered TPI activity on neuronal physiology, linking aberrant TPI function and redox stress to neuronal defects. We used Drosophila mutants expressing a missense allele of the TPI protein, M81T, identified in a previous screen and resulting in an inactive mutant of the TPI protein (TPIM81T , wstd1). We assessed synaptic physiology at the glutamatergic Drosophila neuromuscular junction (NMJ), synapse morphology and behavioural phenotypes, as well as impacts on longevity.

Results: Electrophysiological recordings of evoked and spontaneous excitatory junctional currents, alongside high frequency train stimulations and recovery protocols, were applied to investigate synaptic depletion and subsequent recovery. Single synaptic currents were unaltered in the presence of the wstd1 mutation, but frequencies of spontaneous events were reduced. Wstd1 larvae also showed enhanced vesicle depletion rates at higher frequency stimulation, and subsequent recovery times for evoked synaptic responses were prolonged. A computational model showed that TPI mutant larvae exhibited a significant decline in activity-dependent vesicle recycling, which manifests itself as increased recovery times for the readily-releasable vesicle pool. Confocal images of NMJs showed no morphological or developmental differences between wild-type and wstd1 but TPI mutants exhibited learning impairments as assessed by olfactory associative learning assays.

Discussion: Our data suggests that the wstd1 phenotype is partially due to altered vesicle dynamics, involving a reduced vesicle pool replenishment, and altered endo/exocytosis processes. This may result in learning and memory impairments and neuronal dysfunction potentially also presenting a contributing factor to other reported neuronal phenotypes.

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