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Structure-activity relationship study of trifluoromethylketones: inhibitors of insect juvenile hormone esterase

机译:三氟甲基酮的构效关系研究:昆虫幼激素酯酶抑制剂

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摘要

The juvenile hormone esterase (JHE) regulates juvenile hormone titre in insect hemolymph during its larval development. It has been suggested that JHE could be targeted for use in insect control. This enzyme can also be considered as involved in the phenomenon of endocrine disruption by xenobiotics in beneficial insects. Consequently, there is a need to know the characteristics of the molecules able to act on the JHE. Trifluoromethylketones (TFKs) are the most potent JHE inhibitors found to date anddifferent quantitative structure-activity relationships (QSARs) have been derived for this group of chemicals. In this context, a set of 181 TFKs (118 active and 63 inactive compounds), tested on Trichoplusia ni for their JHE inhibition activity and described by physico-chemical descriptors, was split into different training and test sets to derive structure-activity relationship (SAR) models from support vector classification (SVC). A SVC model including 88 descriptors and derived from a Gaussian kernel was selected for its predictive performances. Another model computed only with 13 descriptors was also selected due to its mechanistic interpretability. This study clearly illustrates the difficulty in capturing the essential structural characteristicsof the TFKs explaining their JHE inhibitory activity.
机译:幼体酯酶(JHE)在昆虫幼虫发育期间调节昆虫血淋巴中的幼体滴度。有人建议将JHE用于昆虫防治。该酶也可以被认为与有益昆虫中的异种生物干扰内分泌的现象有关。因此,需要知道能够作用于JHE的分子的特性。三氟甲基酮(TFKs)是迄今为止发现的最有效的JHE抑制剂,对于这类化学物质,已得出了不同的定量构效关系(QSAR)。在这种情况下,将一组181种TFK(118种活性化合物和63种非活性化合物)在Trichoplusia ni上测试了其JHE抑制活性,并通过理化描述符进行了描述,将其分为不同的训练和测试集以得出结构-活性关系(支持向量分类(SVC)中的SAR)模型。选择具有88个描述符并从高斯核派生的SVC模型以实现预测性能。由于其机械可解释性,还选择了仅用13个描述符计算的另一个模型。这项研究清楚地说明了难以捕获TFK的基本结构特征以解释其JHE抑制活性。

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