首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >p-Alkyl-Benzoyl-CoA Conjugates as Relevant Metabolites of Aromatic Aldehydes With Rat Testicular Toxicity—Studies Leading to the Design of a Safer New Fragrance Chemical
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p-Alkyl-Benzoyl-CoA Conjugates as Relevant Metabolites of Aromatic Aldehydes With Rat Testicular Toxicity—Studies Leading to the Design of a Safer New Fragrance Chemical

机译:P-烷基 - 苯甲酰基-CoA缀合物与大鼠睾丸毒性的芳香醛相关代谢物 - 导致更安全的新香水化学品设计

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Several aromatic aldehydes such as 3-(4-tert-butylphenyl)-2-methylpropanal were shown to adversely affect the reproductive system in male rats following oral gavage dose of?≥?25?mg/kg bw/d. It was hypothesized that these aldehydes are metabolized to benzoic acids such as p-tert-butylbenzoic acid as key toxic principle and that Coenzyme A (CoA) conjugates may be formed from such acids. Here we performed a detailed structure activity relationship study on the formation of benzoic acids from p-alkyl-phenylpropanals and related chemicals in rat hepatocytes in suspension. Formation of CoA conjugates from either p-alkyl-phenylpropanals directly or from their benzoic acid metabolites was further assessed in plated rat hepatocytes using high resolution LC-MS. All of the test chemicals causing reproductive adverse effects in male rats formed p-alkyl-benzoic acids in rat hepatocytes in suspension. Compounds metabolized to p-alkyl-benzoic acids led to accumulation of p-alkyl-benzoyl-CoA conjugates at high and steady levels in plated rat hepatocytes, whereas CoA conjugates of most other xenobiotic acids were only transiently detected in this in vitro system. The correlation between this metabolic fate and the toxic outcome may indicate that accumulation of the alkyl-benzoyl-CoA conjugates in testicular cells could impair male reproduction by adversely affecting CoA-dependent processes required for spermatogenesis. This hypothesis prompted a search for new p-alkyl-phenylpropanal derivatives which do not form benzoic acid metabolites and the corresponding CoA conjugates. It was found that such metabolism did not occur with a derivative containing an o-methyl substituent, ie, 3-(4-isobutyl-2-methylphenyl)propanal. This congener preserved the fragrance quality but lacked the male reproductive toxicity in a 28-day rat study, as predicted from its in vitro metabolism.
机译:在口服饲养剂量的α≥2mg/ kg bw / d之后,显示出几种芳香族醛如3-(4-叔丁基苯基)-2-甲基丙醛醛,在口服饲养剂量ω≥25μmβ2mg/ kg bw / d之后对雄性大鼠的生殖系统产生不利影响。假设这些醛代谢为苯甲酸,例如p-叔丁基苯甲酸作为关键的毒性原理,并且辅酶A(COA)缀合物可以由这种酸形成。在这里,我们对悬浮液中大鼠肝细胞中的P-烷基 - 苯基丙基丙烯酸和相关化学品形成了详细的结构活动关系研究。使用高分辨率LC-MS进一步评估来自P-烷基 - 苯基丙烷的COA缀合物的COA缀合物,通过高分辨率LC-MS在镀大鼠肝细胞中进行进一步评估。所有测试化学品导致雄性大鼠在悬浮液中的雄性大鼠中形成的p-烷基 - 苯甲酸。代谢到p-烷基 - 苯甲酸的化合物导致在镀大鼠肝细胞的高和稳定水平下积聚P-烷基 - 苯甲酰-CoA缀合物,而在该体外系统中仅瞬时检测到大多数其他异黄酸的COA缀合物。这种代谢命运与毒性结果之间的相关性表示,通过对精子发生所需的COA依赖性方法产生不利影响,睾丸细胞中烷基苯甲酰基-CoA缀合物的积累可能会损害雄性繁殖。该假设促进了未形成苯甲酸代谢物和相应的COA缀合物的新的对烷基 - 苯基丙醛衍生物的研究。发现这种代谢不会与含有O-甲基取代基的衍生物,即3-(4-异丁基-2-甲基苯基)丙醛发生。这种同切保存了香料质量,但缺乏28天的大鼠研究中的男性生殖毒性,从其体外代谢预测。

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