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An Information Storage Mechanism: Calcium and Spines

dc.date.accessioned2004-10-04T14:55:06Z
dc.date.accessioned2018-11-24T10:13:21Z
dc.date.available2004-10-04T14:55:06Z
dc.date.available2018-11-24T10:13:21Z
dc.date.issued1984-04-01en_US
dc.identifier.urihttp://hdl.handle.net/1721.1/6405
dc.identifier.urihttp://repository.aust.edu.ng/xmlui/handle/1721.1/6405
dc.description.abstractThis proposal addresses some of the biophysical events possibly underlying fast activity-dependent changes in synaptic efficiency. Dendritic spines in the cortex have attracted increased attention over the last years as a possible locus of cellular plasticity given the large number of studies reporting a close correlation between presynaptic activity (or lack of thereof) and changes in spine shape. This is highlighted by recent reports, showing that the spine cytoplasm contains high levels of actin. Moreover, it has been demonstrated that a high level of intracellular free calcium Ca squared positive, is a prerequisite for various forms of synaptic potentiation. We propose a series of plausible steps, linking presynaptic electrical activity at dendritic spines with a short lasting change in spine geometry. Specifically, we conjecture that the spike-induced excitatory postsynaptic potential triggers an influx of Ca squared positive into the spine, where it will rapidly bind to intracellular calcium buffers such as calmodulin and calcineurin. However, for prolonged or intense presynaptic electrical activity, these buffers will saturate, the free Ca squared positive will then activate the actin/myosin network in the spine neck, reversibly shortening the length of the neck and increasing its diameter. This change in the geometry of the spine will lead to an increase in the synaptic efficiency of the synapse. We will discuss the implication of our proposal for the control of cellular plasticity and its relation to generalized attention and arousal.en_US
dc.format.extent2589811 bytes
dc.format.extent2010346 bytes
dc.language.isoen_US
dc.titleAn Information Storage Mechanism: Calcium and Spinesen_US


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