Chen C, Regehr W G
Department of Neurobiology, Harvard Medical School, Boston, Massachusetts 02115, USA.
J Neurosci. 1997 Nov 15;17(22):8687-94. doi: 10.1523/JNEUROSCI.17-22-08687.1997.
Increases in cAMP have been shown previously to enhance the strength of the granule cell to Purkinje cell synapse. We have examined the mechanisms underlying this enhancement in rat cerebellar brain slices. Elevation of cAMP levels by forskolin increased synaptic currents in a dose-dependent manner. Fluorometric calcium measurements revealed that forskolin did not affect presynaptic calcium influx or resting calcium levels. The waveform of the presynaptic volley was also unaltered, indicating that changes in the presynaptic action potential did not contribute to synaptic enhancement. However, forskolin enhanced the frequency but not the size of spontaneous miniature EPSCs. There was a one-to-one correspondence between increases of spontaneous and evoked neurotransmitter release. These results suggest that forskolin increases release at this synapse via presynaptic mechanisms that do not alter calcium influx. The effect of forskolin on paired-pulse facilitation was examined to assess the relative contributions of changes in the probability of release (p) and changes in the number of functional release sites (n) to this form of enhancement. These experiments suggest that although small changes in n cannot be excluded, most of the enhancement arises from increases in p.
先前已表明,环磷酸腺苷(cAMP)的增加可增强颗粒细胞与浦肯野细胞突触的强度。我们研究了大鼠小脑脑片中这种增强作用的潜在机制。福斯高林提高cAMP水平后,以剂量依赖的方式增加了突触电流。荧光钙测量显示,福斯高林不影响突触前钙内流或静息钙水平。突触前峰电位的波形也未改变,这表明突触前动作电位的变化对突触增强没有作用。然而,福斯高林增加了自发微小兴奋性突触后电流(mEPSC)的频率,但未增加其幅度。自发和诱发神经递质释放的增加之间存在一一对应关系。这些结果表明,福斯高林通过不改变钙内流的突触前机制增加了该突触的释放。研究了福斯高林对双脉冲易化的影响,以评估释放概率(p)的变化和功能性释放位点数量(n)的变化对这种增强形式的相对贡献。这些实验表明,虽然不能排除n有小的变化,但大部分增强来自p的增加。
