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Benzodiazepines: electron affinity, receptors and cell signaling - a multifaceted approach

机译:苯二氮卓类:电子亲和力,受体和细胞信号传导-多方面的方法

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This report entails a multifaceted approach to benzodiazepine (BZ) action, involving electron affinity, receptors, cell signaling and other aspects. Computations of the electron affinities (EAs) of different BZs have been carried out to establish the effect of various substituents on their EA. These computations were undertaken to serve as a first step in determining what role electron transfer (ET) plays in BZ activity. The calculations were conducted on the premise that the nature of the substituent will either decrease or increase the electron density of the benzene ring, thus altering the ability of the molecule to accept an electron. Investigations were performed on the effect of drug protonation on EA. Similarities involving substituent effects in prior electrochemical studies are also discussed. As part of the multifaceted approach, EA is linked to ET, which appears to play a role in therapeutic activity and toxicity. There is extensive literature dealing with the role of receptors in BZ activity. Significant information on receptor involvement was reported more than 40 years ago. Gamma-aminobutyric acid (GABA) is known to be importantly involved. GABA is a probable mediator of BZ effects. BZ and GABA receptors, although not identical, are physiologically linked. Cell signaling is known to play a part in the biochemistry of BZ action. Various factors participated, such as gene expression, allosteric influence, toxic effects and therapeutic action. Evidence points to involvement of EA and ET in the mode of action in cell signaling. Oxidative stress and antioxidant effects are also addressed.
机译:该报告涉及苯二氮卓(BZ)作用的多方面方法,涉及电子亲和力,受体,细胞信号传导和其他方面。已经进行了不同BZ的电子亲和力(EA)的计算,以建立各种取代基对其EA的影响。进行这些计算是确定电子转移(ET)在BZ活性中起什么作用的第一步。计算的前提是取代基的性质会降低或增加苯环的电子密度,从而改变分子接受电子的能力。研究了药物质子化对EA的影响。还讨论了在先前的电化学研究中涉及取代基效应的相似性。作为多方面方法的一部分,EA与ET相关联,而ET似乎在治疗活性和毒性中起作用。有大量文献涉及受体在BZ活性中的作用。关于受体参与的重要信息已有40多年的历史了。已知γ-氨基丁酸(GABA)参与其中。 GABA可能是BZ效应的介体。 BZ和GABA受体虽然不完全相同,但在生理上是相互联系的。已知细胞信号传导在BZ作用的生物化学中起作用。各种因素参与,例如基因表达,变构影响,毒性作用和治疗作用。有证据表明,EA和ET参与了细胞信号转导的作用方式。还解决了氧化应激和抗氧化作用。

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