磷脂酶A2的激活和花生四烯酸等脂质介质在突触的释放:血小板活化因子的作用。

Journal of lipid mediators Pub Date : 1993-03-01
N G Bazan, C F Zorumski, G D Clark
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引用次数: 0

摘要

癫痫发作可通过游离花生四烯酸(AA)和二十二碳六烯酸(DHA)池大小的增加,在分离的突触体中选择性地检测到PLA2的激活。在长期增强过程中,几个实验室对AA及其含氧代谢物的作用进行了探讨。我们研究了另一种PLA2产物,血小板活化因子(PAF, 1- o -烷基-2-乙酰-甘油磷脂胆碱),它也在强烈的突触活动(如癫痫发作)中产生。我们在突触和细胞膜上发现了特定的PAF结合位点。利用大鼠出生后海马突触对,我们已经表明PAF特异性地增加兴奋性神经递质的释放。这种作用是通过突触结合位点引起的,因为选择性的拮抗剂阻断了paf介导的兴奋性神经递质释放的增加。虽然PAF增强诱发兴奋性突触电流,但它不改变gaba介导的抑制性电流。PAF增加自发性兴奋性突触小波的频率,但不增加其幅度。目前尚不清楚积累游离多不饱和脂肪酸的磷脂酶A2是否与产生PAF的磷脂酶A2相同。这种脂质介质对兴奋性突触传递的影响可能是长时程增强、突触可塑性、记忆形成和癫痫发生的关键步骤。
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The activation of phospholipase A2 and release of arachidonic acid and other lipid mediators at the synapse: the role of platelet-activating factor.

Seizures promote PLA2 activation which is selectively detectable in isolated synaptosomes by an increased free arachidonic acid (AA) and docosahexaenoic acid (DHA) pool size. During long-term potentiation, a role of AA and its oxygenated metabolites has been explored in several laboratories. We have studied another PLA2 product, platelet-activating factor (PAF, 1-O-alkyl-2-acetyl-glycerophosphocholine) that is also generated during intense synaptic activity such as seizures. We found specific PAF binding sites in both synaptic and intracellular membranes. Using rat postnatal hippocampal synaptic pairs we have shown that PAF specifically increases the release of excitatory neurotransmitter. This effect is elicited through the synaptic binding site since an antagonist selective for this site blocks the PAF-mediated increase in excitatory neurotransmitter release. Although PAF augments evoked excitatory synaptic currents, it does not alter GABA-mediated inhibitory currents. PAF increases the frequency but not the amplitude of spontaneous excitatory synaptic minis. At present it is not known if the phospholipase A2 that accumulates free polyunsaturated fatty acids is the same as the one that gives rise to PAF. This lipid mediator effect on excitatory synaptic transmission may be a critical step in long term potentiation, synaptic plasticity, memory formation and epileptogenesis.

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