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果蝇细胞色素 P450 酶与杀虫剂抗性相关的同源建模。

Homology modelling of Drosophila cytochrome P450 enzymes associated with insecticide resistance.

机构信息

Department of Biology and Biochemistry, University of Bath, Bath, UK.

出版信息

Pest Manag Sci. 2010 Oct;66(10):1106-15. doi: 10.1002/ps.1986.

Abstract

BACKGROUND

Overexpression of the cytochrome P450 gene Cyp6g1 confers resistance against DDT and a broad range of other insecticides in Drosophila melanogaster Meig. In the absence of crystal structures of CYP6G1 or complexes with its substrates, structural studies rely on homology modelling and ligand docking to understand P450-substrate interactions.

RESULTS

Homology models are presented for CYP6G1, a P450 associated with resistance to DDT and neonicotinoids, and two other enzymes associated with insecticide resistance in D. melanogaster, CYP12D1 and CYP6A2. The models are based on a template of the X-ray structure of the phylogenetically related human CYP3A4, which is known for its broad substrate specificity. The model of CYP6G1 has a much smaller active site cavity than the template. The cavity is also 'V'-shaped and is lined with hydrophobic residues, showing high shape and chemical complementarity with the molecular characteristics of DDT. Comparison of the DDT-CYP6G1 complex and a non-resistant CYP6A2 homology model implies that tight-fit recognition of this insecticide is important in CYP6G1. The active site can accommodate differently shaped substrates ranging from imidacloprid to malathion but not the pyrethroids permethrin and cyfluthrin.

CONCLUSION

The CYP6G1, CYP12D1 and CYP6A2 homology models can provide a structural insight into insecticide resistance in flies overexpressing P450 enzymes with broad substrate specificities.

摘要

背景

细胞色素 P450 基因 Cyp6g1 的过度表达赋予了黑腹果蝇对滴滴涕和其他多种杀虫剂的抗性。在缺乏 CYP6G1 的晶体结构或与其底物复合物的情况下,结构研究依赖于同源建模和配体对接来理解 P450-底物相互作用。

结果

本文提出了与滴滴涕和新烟碱类杀虫剂抗性相关的 P450 酶 CYP6G1 以及与黑腹果蝇中杀虫剂抗性相关的另外两种酶 CYP12D1 和 CYP6A2 的同源模型。这些模型基于与系统发育相关的人 CYP3A4 的 X 射线结构模板,该模板以其广泛的底物特异性而闻名。CYP6G1 的模型具有比模板小得多的活性位点腔。该腔也是“V”形的,由疏水性残基排列,与滴滴涕的分子特征具有高度的形状和化学互补性。将 DDT-CYP6G1 复合物与非抗性 CYP6A2 同源模型进行比较表明,这种杀虫剂的紧密-fit 识别对于 CYP6G1 很重要。活性位点可以容纳从吡虫啉到马拉硫磷的不同形状的底物,但不能容纳拟除虫菊酯类杀虫剂氯菊酯和氟氯氰菊酯。

结论

CYP6G1、CYP12D1 和 CYP6A2 的同源模型可以为过度表达具有广泛底物特异性的 P450 酶的果蝇中的杀虫剂抗性提供结构见解。

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