McLennan H
Prog Neurobiol. 1983;20(3-4):251-71. doi: 10.1016/0301-0082(83)90004-7.
On the basis largely of neuropharmacological analysis, three different receptors mediating neuronal excitation can be identified. The first is activated by quisqualate and other "flexible" molecules including L-glutamate and appears to bind its ligands in a folded configuration. The second is excited by NMDA and has a more extended conformation, the spacing between the amino and the omega-carboxylate groups being the determinant of specificity. The third type accepts kainate and appears to possess a reactive site for the unsaturated side chain which is essential to the operation of this receptor. All three classes appear to be implicated in synaptic events [although some kainate receptors at least are certainly extra-synaptic (Watkins et al., 1981)] and each appears to activate different ionophores in neuronal membranes. Of the endogenous amino acids which may function as synaptic transmitters, L-glutamate and L-cysteate seem to react preferentially with quisqualate receptors (McLennan and Lodge, 1979), while L-aspartate is more of a mixed agonist capable of reaction both with quisqualate and with the NMDA types. Whether folate has a physiological role involving kainate receptors is unknown; and the same is true of any action possessed by quinolinate. The fact that there are amino acid excitants which are pharmacologically distinct from those reacting with any of the three best known receptors suggests that at least one more class of receptor may also exist, but no further information is available at the present time. Other sites with which the pharmacologically active acidic amino acids react are identifiable neurochemically in membrane preparations derived from tissues of the central nervous system. Kinetic studies and analysis of inhibition of sodium-independent binding indicate that there are sites which accept glutamate, others binding aspartate and a third which binds kainate. However, the first does not correspond completely to the quisqualate excitatory receptor, and NMDA does not react with any of the binding sites. It is difficult to conclude then that any of these binding sites can be fully identified with the excitatory receptors. Finally, there are a number of systems which in their patterns of activity again appear completely distinct, but which presumably mediate uptake of amino acids.(ABSTRACT TRUNCATED AT 400 WORDS)
主要基于神经药理学分析,可以识别出三种介导神经元兴奋的不同受体。第一种受体由喹啉酸和其他“柔性”分子(包括L-谷氨酸)激活,并且似乎以折叠构象结合其配体。第二种受体由N-甲基-D-天冬氨酸(NMDA)激活,具有更伸展的构象,氨基和ω-羧基之间的间距是特异性的决定因素。第三种受体接受海人藻酸,并且似乎具有对不饱和侧链的反应位点,这对该受体的运作至关重要。所有这三类受体似乎都与突触事件有关[尽管至少一些海人藻酸受体肯定位于突触外(沃特金斯等人,1981年)],并且每一种似乎都能激活神经元膜中的不同离子载体。在可能作为突触递质起作用的内源性氨基酸中,L-谷氨酸和L-半胱氨酸似乎优先与喹啉酸受体反应(麦克伦南和洛奇,1979年),而L-天冬氨酸更像是一种混合激动剂,能够与喹啉酸受体和NMDA受体类型都发生反应。叶酸是否具有涉及海人藻酸受体的生理作用尚不清楚;喹啉酸的任何作用也是如此。存在与三种最知名受体中任何一种反应的药理学上不同的氨基酸兴奋剂,这一事实表明可能还存在至少一类受体,但目前尚无更多信息。在源自中枢神经系统组织的膜制剂中,可以通过神经化学方法鉴定出与具有药理活性的酸性氨基酸反应的其他位点。动力学研究和对非钠依赖性结合抑制的分析表明,存在接受谷氨酸的位点、其他结合天冬氨酸的位点以及第三种结合海人藻酸的位点。然而,第一个位点并不完全对应于喹啉酸兴奋性受体,并且NMDA不与任何结合位点反应。因此,很难得出这些结合位点中的任何一个都能与兴奋性受体完全等同的结论。最后,有许多系统,它们的活动模式再次显得完全不同,但大概介导氨基酸的摄取。(摘要截取自400字)
