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Ca2+ Regulates the Drosophila Stoned-A and Stoned-B Proteins Interaction with the C2B Domain of Synaptotagmin-1

机译:Ca2 +调节果蝇Stoneaptagmin-1的C2B域的果蝇Stoned-A和Stoned-B蛋白相互作用。

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摘要

The dicistronic Drosophila stoned gene is involved in exocytosis and/or endocytosis of synaptic vesicles. Mutations in either stonedA or stonedB cause a severe disruption of neurotransmission in fruit flies. Previous studies have shown that the coiled-coil domain of the Stoned-A and the µ-homology domain of the Stoned-B protein can interact with the C2B domain of Synaptotagmin-1. However, very little is known about the mechanism of interaction between the Stoned proteins and the C2B domain of Synaptotagmin-1. Here we report that these interactions are increased in the presence of Ca2+. The Ca2+-dependent interaction between the µ-homology domain of Stoned-B and C2B domain of Synaptotagmin-1 is affected by phospholipids. The C-terminal region of the C2B domain, including the tryptophan-containing motif, and the Ca2+ binding loop region that modulate the Ca2+-dependent oligomerization, regulates the binding of the Stoned-A and Stoned-B proteins to the C2B domain. Stoned-B, but not Stoned-A, interacts with the Ca2+-binding loop region of C2B domain. The results indicate that Ca2+-induced self-association of the C2B domain regulates the binding of both Stoned-A and Stoned-B proteins to Synaptotagmin-1. The Stoned proteins may regulate sustainable neurotransmission in vivo by binding to Ca2+-bound Synaptotagmin-1 associated synaptic vesicles.
机译:双顺反子果蝇结石基因参与突触小泡的胞吐作用和/或内吞作用。 stonedA或stonedB中的突变会导致果蝇神经传递的严重破坏。先前的研究表明,Stoned-A的卷曲螺旋结构域和Stoned-B蛋白的μ同源结构域可以与Synaptotagmin-1的C2B结构域相互作用。但是,人们对Stoned蛋白与Synaptotagmin-1的C2B结构域之间相互作用的机制了解甚少。在这里我们报告说,在Ca 2 + 的存在下,这些相互作用增加了。 Stoned-B的μ同源结构域与Synaptotagmin-1的C2B结构域之间的Ca 2 + 依赖性相互作用受磷脂影响。 C2B域的C端区域(包括含色氨酸的基序)和调节Ca 2 + 依赖性寡聚的Ca 2 + 结合环区域可调节Stoned-A和Stoned-B蛋白与C2B结构域的结合。 Stoned-B,而不是Stoned-A与C2B域的Ca 2 + 结合环区域相互作用。结果表明,Ca 2 + 诱导的C2B域自缔合调节了Stoned-A和Stoned-B蛋白与Synaptotagmin-1的结合。 Stoned蛋白可能通过结合Ca 2 + 结合的Synaptotagmin-1相关突触小泡而调节体内可持续的神经传递。

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