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PSD-95 promotes the stabilization of young synaptic contacts

机译:PSD-95促进年轻突触接触的稳定

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Maintaining a population of stable synaptic connections is probably of critical importance for the preservation of memories and functional circuitry, but the molecular dynamics that underlie synapse stabilization is poorly understood. Here, we use simultaneous time-lapse imaging of post synaptic density-95 (PSD-95) and Ca~(2+)/calmodulin-dependent protein kinase II (CaMKII) to investigate the dynamics of protein composition at axodendritic (AD) contacts. Our data reveal that this composition is highly dynamic, with both proteins moving into and out of the same synapse independently, so that synapses cycle rapidly between states in which they are enriched for none, one or both proteins. We assessed how PSD-95 and CaMKII interact at stable and transient AD sites and found that both phospho-CaMKII and PSD-95 are present more often at stable than labile contacts. Finally, we found that synaptic contacts are more stable in older neurons, and this process can be mimicked in younger neurons by overexpression of PSD-95. Taken together, these data show that synaptic protein composition is highly variable over a time-scale of hours, and that PSD-95 is probably a key synaptic protein that promotes synapse stability.
机译:维持稳定的突触连接群对于保存记忆和功能电路可能至关重要,但是对突触稳定基础的分子动力学知之甚少。在这里,我们使用突触后密度95(PSD-95)和Ca〜(2 +)/钙调蛋白依赖性蛋白激酶II(CaMKII)的同步延时成像来研究轴突(AD)接触时蛋白质组成的动力学。 。我们的数据表明,这种组成是高度动态的,两种蛋白质都独立地移入和移出同一突触,因此突触在它们不富集一种或两种蛋白质的状态之间快速循环。我们评估了PSD-95和CaMKII如何在稳定和短暂的AD位点相互作用,并且发现磷酸CaMKII和PSD-95都比不稳定的接触更稳定地存在。最后,我们发现突触接触在较老的神经元中更稳定,并且该过程可以通过过表达PSD-95在较年轻的神经元中进行模仿。综上所述,这些数据表明,在数小时的时间内,突触蛋白的组成高度可变,并且PSD-95可能是促进突触稳定性的关键突触蛋白。

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