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首页> 外文期刊>Anesthesia and Analgesia: Journal of the International Anesthesia Research Society >The anesthetic-like effects of diverse compounds on wild-type and mutant gamma-aminobutyric acid type A and glycine receptors.
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The anesthetic-like effects of diverse compounds on wild-type and mutant gamma-aminobutyric acid type A and glycine receptors.

机译:多种化合物对野生型和突变型A型γ-氨基丁酸和甘氨酸受体的麻醉作用。

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INTRODUCTION: No theory of inhaled anesthetic action requires volatility of the anesthetic to accomplish the biophysical interaction of anesthetic with biological target. The identification of mutations that attenuate the effect of inhaled anesthetics on various receptors raises the possibility that nonvolatile compounds with anesthetic effects can be identified with the aid of these receptors. In previous studies, we identified compounds that were either charged or had an exceptionally low vapor pressure and which modulated anesthetic-sensitive receptors in a manner similar to inhaled anesthetics. We tested whether these, and another charged compound, shared a common mechanism with volatile anesthetics, by comparing their effect on wild-type gamma-aminobutyric acid type A (GABA(A)) or glycine receptors and mutant receptors that were engineered to be relatively resistant to inhaled anesthetics. METHODS: The effect of beta-hydroxybutyric acid, ammonium chloride, diethylhexyl phthalate, and GABA were tested on homomeric alpha1 and mutant alpha1 (S267I) glycine receptors. The effect of sodium dodecyl sulfate and glycine were tested on alpha1 b2 gamma2s and mutant alpha1(S270I) beta2 gamma2s GABA(A) receptors. Receptors were expressed in Xenopus laevis oocytes and studied using two-electrode voltage clamping. For both GABA(A) and glycine receptors, isoflurane and ethanol were used as positive controls and propofol as a negative control (i.e., unaffected by the mutation). RESULTS: Beta-hydroxybutyric acid, ammonium chloride, diethylhexyl phthalate, and GABA all enhanced glycine receptor function. This effect was reduced by the S267I mutations. Sodium dodecyl sulfate and glycine enhanced GABA(A) receptor function, and the S270I mutation attenuated this effect. CONCLUSION: These findings support the hypothesis that the compounds studied modulate GABA(A) or glycine receptors by a mechanism similar to that of isoflurane and ethanol. Comparing the effect of drugs on anesthetic-sensitive wild-type receptors with relatively less sensitive mutant receptors may help identify compounds with anesthetic effects.
机译:简介:吸入麻醉作用的理论都不需要麻醉剂的挥发性即可完成麻醉剂与生物靶标的生物物理相互作用。鉴定减弱吸入麻醉剂对各种受体作用的突变,增加了可以借助这些受体鉴定具有麻醉作用的非挥发性化合物的可能性。在以前的研究中,我们确定了带电或蒸气压极低且以类似于吸入麻醉药的方式调节麻醉药敏感性受体的化合物。我们通过比较它们对野生型A型γ-氨基丁酸(GABA(A))或设计为相对工程化的甘氨酸受体和突变受体的作用,来测试这些化合物和另一种带电荷化合物是否与挥发性麻醉剂共有相同的机理耐吸入麻醉药。方法:测试了β-羟基丁酸,氯化铵,邻苯二甲酸二乙基己酯和GABA对同型α1和突变体α1(S267I)甘氨酸受体的影响。测试了十二烷基硫酸钠和甘氨酸对alpha1 b2 gamma2s和突变体alpha1(S270I)beta2 gamma2s GABA(A)受体的作用。受体在非洲爪蟾卵母细胞中表达,并使用两电极电压钳制研究。对于GABA(A)和甘氨酸受体,异氟烷和乙醇用作阳性对照,丙泊酚用作阴性对照(即不受突变影响)。结果:β-羟基丁酸,氯化铵,邻苯二甲酸二乙基己酯和GABA均增强了甘氨酸受体的功能。 S267I突变降低了这种作用。十二烷基硫酸钠和甘氨酸增强GABA(A)受体功能,而S270I突变减弱了这种作用。结论:这些发现支持以下假设:所研究的化合物通过类似于异氟烷和乙醇的机制来调节GABA(A)或甘氨酸受体。将药物对麻醉敏感的野生型受体的药效与敏感性相对较低的突变受体进行比较,可能有助于鉴定具有麻醉作用的化合物。

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