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受体系统反应动力学揭示了天然小鼠和重组人GABAA受体的功能亚型。

Receptor system response kinetics reveal functional subtypes of native murine and recombinant human GABAA receptors.

作者信息

McClellan A M, Twyman R E

机构信息

Programs in Neuroscience and in Human Molecular Biology and Genetics, Departments of Neurology and Pharmacology, University of Utah, Salt Lake City, UT 84112, USA.

出版信息

J Physiol. 1999 Mar 15;515 ( Pt 3)(Pt 3):711-27. doi: 10.1111/j.1469-7793.1999.711ab.x.

DOI:10.1111/j.1469-7793.1999.711ab.x
PMID:10066899
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2269184/
Abstract
  1. Regional distinctions in GABA type A (GABAA) miniature IPSC responses are thought to be determined by postsynaptic receptor composition. The kinetics of receptor activation and deactivation were studied using rapid exchange (100 micros) of GABA at excised patches containing recombinant (alpha1beta1gamma2 or alpha2beta1gamma2) and native (cortical) GABAA receptors. 2. Receptors activated by brief (< 1 ms) pulses of GABA demonstrated a characteristic current response, hereby referred to as the 'receptor system response'. System response properties included agonist concentration-dependent peak amplitudes and concentration-independent maximal rates of activation and deactivation. Receptor subtypes were characterized functionally and phenotyped using the system response characteristics. 3. System responses obtained for alpha1beta1gamma2 receptors exhibited a single phenotype while alpha2beta1gamma2 receptors exhibited either a predominant slow deactivation (type I) or a relatively infrequent faster (type II) phenotype. Receptor system responses of alpha2beta1gamma2 receptors reached peak currents twice as fast as those of alpha1beta1gamma2 receptors (0.5 versus 1.0 ms) but decayed 2 or 6 times more slowly (taulong of approximately 190 and 62 ms for type I and II alpha2beta1gamma2, and approximately 34 ms for alpha1beta1gamma2 receptors). 4. Receptor system responses from cultured fetal mouse cortical neurons could be statistically separated and classified into five major types with little intragroup variability, primarily based on variations in the current deactivation phases. 5. Receptors subjected to pharmacological modulation exhibited alterations in system response properties consistent with known mechanisms of action, such that distinctions between binding and gating modulations were possible. 6. Brief agonist exposure places limits on receptor activation and deactivation response kinetics. Consequently, receptor system responses may be used to characterize and functionally phenotype an excised patch receptor population. Furthermore, since synaptic exposure to transmitter is postulated to be similarly brief, IPSC kinetics may reflect a functional fingerprint of synaptic receptors.
摘要
  1. γ-氨基丁酸A型(GABAA)微小抑制性突触后电流反应的区域差异被认为是由突触后受体组成决定的。在含有重组(α1β1γ2或α2β1γ2)和天然(皮质)GABAA受体的膜片上,通过快速交换(100微秒)γ-氨基丁酸来研究受体激活和失活的动力学。2. 由短暂(<1毫秒)的γ-氨基丁酸脉冲激活的受体表现出特征性电流反应,在此称为“受体系统反应”。系统反应特性包括激动剂浓度依赖性峰值幅度以及与浓度无关的最大激活和失活速率。利用系统反应特性对受体亚型进行功能表征和表型鉴定。3. α1β1γ2受体获得的系统反应表现出单一表型,而α2β1γ2受体则表现出主要的缓慢失活(I型)或相对少见的较快失活(II型)表型。α2β1γ2受体的受体系统反应达到峰值电流的速度是α1β1γ2受体的两倍(0.5毫秒对1.0毫秒),但衰减速度慢2至6倍(I型和II型α2β1γ2的τlong约为190和62毫秒,α1β1γ2受体约为34毫秒)。4. 培养的胎鼠皮质神经元的受体系统反应在统计学上可分为五种主要类型,组内变异性很小,主要基于电流失活阶段的变化。5. 接受药理调制的受体在系统反应特性上表现出与已知作用机制一致的改变,从而有可能区分结合调制和门控调制。6. 短暂的激动剂暴露对受体激活和失活反应动力学施加了限制。因此,受体系统反应可用于表征和功能鉴定膜片上的受体群体。此外,由于假定突触对递质的暴露同样短暂,抑制性突触后电流动力学可能反映突触受体的功能指纹。

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