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分离锌在重组 N-甲基-D-天冬氨酸受体上的双重作用。

Separating dual effects of zinc at recombinant N-methyl-D-aspartate receptors.

作者信息

Williams K

机构信息

Department of Pharmacology, University of Pennsylvania, School of Medicine, Philadelphia 19104-6084, USA.

出版信息

Neurosci Lett. 1996 Aug 30;215(1):9-12. doi: 10.1016/s0304-3940(96)12924-4.

Abstract

The effects of Zn2+ on recombinant N-methyl-D-aspartate (NMDA) receptors expressed in Xenopus oocytes were examined. Zn2+ inhibited macroscopic currents induced by NMDA at both NR1/NR2B and NR1/NR2A receptors. At NR1/NR2B receptors the Zn2+ concentration-inhibition curve was monophasic, with an apparent affinity for Zn2/ of 1.6 microM, and inhibition by Zn2+ was not voltage-dependent. In contrast, the Zn2+ concentration-inhibition curve at NR1/NR2A receptors was biphasic, with high (Ki = 0.08 microM) and low (Ki = 30 microM) affinity components. The high affinity component produced a maximal inhibition of 45% of macroscopic NMDA currents and was not voltage-dependent. Thus, Zn2+ is more potent in producing voltage-independent block at NR1/NR2A than at NR1/NR2B receptors, but the maximal effect of Zn2+ is smaller at NR1/NR2A than at NR1/NR2B receptors. The low affinity component of Zn2+ inhibition at NR1/NR2A receptors was voltage-dependent and may represent an open-channel blocking effect of Zn2+. Differential effects of Zn2+ at recombinant NMDA receptors containing different NR2 subunits provide a potential marker for distinguishing subtypes of native NMDA receptors and for dissecting the site and mechanism of action of Zn2+ at these receptors.

摘要

研究了锌离子(Zn2+)对非洲爪蟾卵母细胞中表达的重组N-甲基-D-天冬氨酸(NMDA)受体的影响。Zn2+抑制了NR1/NR2B和NR1/NR2A受体处由NMDA诱导的宏观电流。在NR1/NR2B受体处,Zn2+浓度-抑制曲线是单相的,对Zn2+的表观亲和力为1.6微摩尔,且Zn2+的抑制不依赖电压。相比之下,NR1/NR2A受体处的Zn2+浓度-抑制曲线是双相的,具有高亲和力(Ki = 0.08微摩尔)和低亲和力(Ki = 30微摩尔)成分。高亲和力成分对宏观NMDA电流产生了45%的最大抑制,且不依赖电压。因此,Zn2+在NR1/NR2A受体处产生非电压依赖性阻断的效力比在NR1/NR2B受体处更强,但Zn2+在NR1/NR2A受体处的最大效应比在NR1/NR2B受体处更小。NR1/NR2A受体处Zn2+抑制的低亲和力成分依赖电压,可能代表了Zn2+的开放通道阻断作用。Zn2+在含有不同NR2亚基的重组NMDA受体上的不同作用,为区分天然NMDA受体亚型以及剖析Zn2+在这些受体上的作用位点和机制提供了一个潜在的标志物。

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