C57BL/6小鼠脑中N-甲基-4-苯基-1,2,3,6-四氢吡啶（MPTP）结合位点的表征：单胺氧化酶抑制剂和σ配体对MPTP和σ结合位点的相互作用

Characterization of N-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) binding sites in C57BL/6 mouse brain: mutual effects of monoamine oxidase inhibitors and sigma ligands on MPTP and sigma binding sites.

作者信息

Itzhak Y, Mash D, Zhang S H, Stein I

机构信息

Department of Biochemistry and Molecular Biology, REPSCEND Laboratories, University of Miami School of Medicine, Florida 33101.

出版信息

Mol Pharmacol. 1991 Mar;39(3):385-93.

PMID:1848660

Abstract

N-Methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP) induces Parkinson-like symptoms in humans, nonhuman primates, and mice. Several studies suggest that MPTP is metabolized by monoamine oxidase (MAO) type B to yield N-methyl-4-phenyl-pyridinium (MPP+), which is responsible for the neurotoxic effects of the drug. In the present study, the pharmacological properties of [3H]MPTP binding sites in C57BL/6 mouse brain membranes were investigated, and a possible relationship to the sigma binding sites was examined. Both equilibrium binding experiments and kinetic assays indicate that [3H]MPTP labels two distinct binding sites in C57BL/6 mouse brain. The high affinity [3H]MPTP binding sites (Kd = 13 nM) are selectively blocked by the MAO type A inhibitor clorgyline, and the residual low affinity [3H]MPTP sites (Kd = 1100 nM) display the pharmacological specificity of MAO-B binding sites. In contrast, the low affinity [3H]MPTP binding sites are blocked by the selective MAO-B inhibitor (-)-deprenyl, and the drug-specificity profile of the remaining high affinity sites is consistent with the properties of MAO-A binding sites. The affinities of several MAO inhibitors tested and of MPTP for the high affinity MPTP/MAO-A binding sites correlate well (r = 0.96) with their affinities for the sigma binding sites labeled with [(+)-[3H]-3-PPP]. The sigma receptor ligand (+)-3-PPP displays moderately high affinity for the MPTP/MAO-A binding sites but negligible affinity for MPTP/MAO-B sites. Moreover, (+)-3-PPP alters the dissociation kinetics of MPTP from the high affinity MPTP/MAO-A sites. The finding that [3H]MPTP labels MAO-B sites supports the hypothesis that the drug is a substrate for these enzyme binding sites. However, the finding that the high affinity sites, labeled by [3H] MPTP, are particularly sensitive to MAO-A inhibitors, which also display high affinity for the sigma binding sites, may suggest a possible relationship between MAO-A and sigma binding sites. In turn, the kinetic experiments imply that sigma ligands [i.e., (+)-3-PPP] may allosterically modulate the binding to MAO-A binding sites.

摘要

N-甲基-4-苯基-1,2,3,6-四氢吡啶（MPTP）可在人类、非人灵长类动物和小鼠中诱发帕金森样症状。多项研究表明，MPTP经B型单胺氧化酶（MAO）代谢生成N-甲基-4-苯基吡啶鎓（MPP+），该物质是造成该药物神经毒性作用的原因。在本研究中，对C57BL/6小鼠脑膜中[3H]MPTP结合位点的药理学特性进行了研究，并检测了其与σ结合位点的可能关系。平衡结合实验和动力学分析均表明，[3H]MPTP在C57BL/6小鼠脑中标记出两个不同的结合位点。高亲和力的[3H]MPTP结合位点（Kd = 13 nM）被A型单胺氧化酶抑制剂氯吉兰选择性阻断，剩余的低亲和力[3H]MPTP位点（Kd = 1100 nM）表现出MAO-B结合位点的药理学特异性。相反，低亲和力的[3H]MPTP结合位点被选择性MAO-B抑制剂（-）-司来吉兰阻断，其余高亲和力位点的药物特异性谱与MAO-A结合位点的特性一致。所测试的几种MAO抑制剂以及MPTP对高亲和力MPTP/MAO-A结合位点的亲和力与它们对用[（+）-[3H]-3-PPP]标记的σ结合位点的亲和力高度相关（r = 0.96）。σ受体配体（+）-3-PPP对MPTP/MAO-A结合位点表现出中等程度的高亲和力，但对MPTP/MAO-B位点的亲和力可忽略不计。此外，（+）-3-PPP改变了MPTP从高亲和力MPTP/MAO-A位点的解离动力学。[3H]MPTP标记MAO-B位点这一发现支持了该药物是这些酶结合位点底物的假说。然而，[3H]MPTP标记的高亲和力位点对MAO-A抑制剂特别敏感，而MAO-A抑制剂对σ结合位点也表现出高亲和力，这一发现可能提示MAO-A与σ结合位点之间存在可能的关系。相应地，动力学实验表明σ配体[即（+）-3-PPP]可能对MAO-A结合位点的结合具有变构调节作用。