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首页> 外文期刊>Medicinal chemistry >Exploring the relationship of drug-induced neutrophil immaturity & haematological toxicity to drug chemistry using quantitative structure-activity models.
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Exploring the relationship of drug-induced neutrophil immaturity & haematological toxicity to drug chemistry using quantitative structure-activity models.

机译:使用定量结构-活性模型探索药物诱导的中性粒细胞不成熟和血液学毒性与药物化学的关系。

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摘要

An investigation of the relationships between physicochemical features of ten antipsychotic drugs and previously reported influence of these drugs on neutrophil maturity was made. A quantitative structure-activity relations (QSAR) approach was adopted, in which several numerical parameters describing physicochemical characteristics of the antipsychotics were estimated. Possible connections between these parameters and neutrophil maturity were explored. Influence of drug physicochemistry on the incidence of agranulocytosis and neutropenia reported in the literature was documented. Overall it was found that drugs with the greatest tendency to induce neutrophil immaturity (chlorpromazine, clozapine and olanzapine) also showed the greatest tendency to cause agranulocytosis and neutropenia. Moreover marked induction of neutrophil immaturity occurred with compounds of moderately amphipathic character, whose amphipathic indices (AI) fell in the range 3-5; higher or lower AI values correlated with less immaturity. Consideration of the QSAR findings suggest that toxicity could be associated with selective uptake into the most fluid intracellular membranes, those of the endoplasmic reticulum and the outer mitochondrial membrane. The AI hazard zone (AI = 3-5) does constitute a predictive tool to assess risk of agranulocytosis and neutropenia arising from antipsychotic and other psychoactive drugs - and not only risk arising from medication but also from experimental or even proposed compounds.
机译:研究了十种抗精神病药的理化特征与先前报道的这些药物对中性粒细胞成熟的影响之间的关系。采用定量构效关系(QSAR)方法,其中估计了描述抗精神病药理化特性的几个数值参数。探索了这些参数与中性粒细胞成熟度之间的可能联系。文献中报道了药物理化对粒细胞缺乏症和中性粒细胞减少症发生率的影响。总的来说,发现诱导中性粒细胞不成熟的趋势最大的药物(氯丙嗪,氯氮平和奥氮平)也具有引起粒细胞缺乏和中性粒细胞减少的最大趋势。此外,中度两亲性化合物的中性粒细胞未成熟明显诱导,其两亲性指数(AI)在3-5范围内;较高或较低的AI值与较少的未成熟度相关。对QSAR研究结果的考虑表明,毒性可能与选择性吸收大多数流体细胞内膜,内质网和线粒体外膜有关。 AI危险区(AI = 3-5)确实是评估抗精神病药和其他精神活性药物引起的粒细胞缺乏和中性粒细胞减少症风险的预测工具-不仅是药物引起的风险,还包括实验甚至是拟议的化合物引起的风险。

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