Substituted quinolines as inhibitors of L-glutamate transport into synaptic vesicles

被引:51
|
作者
Bartlett, RD
Esslinger, CS
Thompson, CM
Bridges, RJ [1 ]
机构
[1] Univ Montana, Dept Pharmaceut Sci, Missoula, MT 59812 USA
[2] Univ Montana, Dept Chem, Missoula, MT 59812 USA
关键词
glutamate; synaptic vesicles; transport; kynurenate; xanthurenate;
D O I
10.1016/S0028-3908(98)00080-X
中图分类号
Q189 [神经科学];
学科分类号
071006 ;
摘要
This study investigated the structure-activity relationships and kinetic properties of a library of kynurenate analogues as inhibitors of H-3-L-glutamate transport into rat forebrain synaptic vesicles. The lack of inhibitory activity observed with the majority of the monocyclic pyridine derivatives suggested that the second aromatic ring of the quinoline-based compounds played a significant role in binding to the transporter. A total of two kynurenate derivatives, xanthurenate and 7-chloro-kynurenate, differing only in the carbocyclic ring substituents, were identified as potent competitive inhibitors: exhibiting K-i values of 0.19 and 0.59 mM, respectively. The K-m value for L-glutamate was found to be 2.46 mM. Parallel experiments demonstrated that while none of the kynurenate analogues tested effectively inhibited the synaptosomal transport of H-3-D-aspartate, some cross-reactivity was observed with the EAA ionotropic receptors. Molecular modeling studies were carried out with the identified inhibitors and glutamate in an attempt to preliminarily define the pharmacophore of the vesicular transporter It is hypothesized that the ability of the kynurenate analogues to bind to the transporter may be tied to the capacity of the quinoline carbocyclic ring to mimic the negative charge of the gamma-carboxylate of glutamate. A total of two low energy solution conformers of glutamate were identified that exhibited marked functional group overlap with the most potent inhibitor, xanthurenate. These results help to further refine the pharmacological specificity of the glutamate binding site on the vesicular transporter and identify a series of inhibitors with which to investigate transporter function. (C) 1998 Elsevier Science Ltd. All rights reserved.
引用
收藏
页码:839 / 846
页数:8
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