Mechanisms and significance of spike-timing dependent plasticity

被引:0
|
作者
Uma R. Karmarkar
Mark T. Najarian
Dean V. Buonomano
机构
[1] Departments of Neurobiology and Psychology,
[2] and Brain Research Institute,undefined
[3] University of California Los Angeles,undefined
[4] Box 951763,undefined
[5] Los Angeles,undefined
[6] CA 90095,undefined
[7] USA,undefined
来源
Biological Cybernetics | 2002年 / 87卷
关键词
Depression; NMDA; Time Window; NMDA Receptor; Experimental Parameter;
D O I
暂无
中图分类号
学科分类号
摘要
 Hebb's original postulate left two important issues unaddressed: (i) what is the effective time window between pre- and postsynaptic activity that will result in potentiation? and (ii) what is the learning rule that underlies decreases in synaptic strength? While research over the past 2 decades has addressed these questions, several studies within the past 5 years have shown that synapses undergo long-term depression (LTD) or long-term potentiation (LTP) depending on the order of activity in the pre- and postsynaptic cells. This process has been referred to as spike-timing dependent plasticity (STDP). Here we discuss the experimental data on STDP, and develop models of the mechanisms that may underlie it. Specifically, we examine whether the standard model of LTP and LTD in which high and low levels of Ca2+ produce LTP and LTD, respectively, can also account for STDP. We conclude that the standard model can account for a type of STDP in which, counterintuitively, LTD will be observed at some intervals in which the presynaptic cell fires before the postsynaptic cell. This form of STDP will also be sensitive to parameters such as the presence of an afterdepolarization following an action potential. Indeed, the sensitivity of this type of STDP to experimental parameters suggests that it may not play an important physiological role in vivo. We suggest that more robust forms of STDP, which do not exhibit LTD at pre–before–post intervals, are not accounted for by the standard model, and are likely to rely on a second coincidence detector in addition to the NMDA receptor.
引用
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页码:373 / 382
页数:9
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