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Neurexin and Neuroligin-based adhesion complexes drive axonal arborisation growth independent of synaptic activity

机译:神经毒素和基于Neuroligin的粘附复合物驱动轴突乔化生长而与突触活性无关

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Building arborisations of the right size and shape is fundamental for neural network function. Live imaging in vertebrate brains strongly suggests that nascent synapses are critical for branch growth during development. The molecular mechanisms underlying this are largely unknown. Here we present a novel system in Drosophila for studying the development of complex arborisations live, in vivo during metamorphosis. In growing arborisations we see branch dynamics and localisations of presynaptic proteins very similar to the ‘synaptotropic growth’ described in fish/frogs. These accumulations of presynaptic proteins do not appear to be presynaptic release sites and are not paired with neurotransmitter receptors. Knockdowns of either evoked or spontaneous neurotransmission do not impact arbor growth. Instead, we find that axonal branch growth is regulated by dynamic, focal localisations of Neurexin and Neuroligin. These adhesion complexes provide stability for filopodia by a ‘stick-and-grow’ based mechanism wholly independent of synaptic activity.
机译:建立正确大小和形状的树状结构是神经网络功能的基础。脊椎动物大脑中的实时成像强烈表明,新生突触对于发育过程中分支的生长至关重要。潜在的分子机制在很大程度上尚不清楚。在这里,我们在果蝇中提出了一个新的系统,用于研究在变态过程中体内活体进行复杂乔木化的过程。在生长的乔木中,我们看到突触前蛋白的分支动态和定位与鱼/青蛙中描述的“突触生长”非常相似。突触前蛋白的这些积累似乎不是突触前释放位点,并且不与神经递质受体配对。诱发或自发的神经传递的敲低并不影响乔木的生长。相反,我们发现轴突分支的生长受Neurexin和Neuroligin的动态,局灶性局部调节。这些粘附复合物通过完全独立于突触活性的基于“粘着生长”的机制为丝状伪足提供稳定性。

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