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Functional characterization of NADPH-cytochrome P450 reductase from Bactrocera dorsalis: Possible involvement in susceptibility to malathion

机译:桔小实蝇NADPH细胞色素P450还原酶的功能表征:可能参与马拉硫磷的敏感性

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摘要

NADPH cytochrome P450 reductase (CPR) is essential for cytochrome P450 catalysis, which is important in the detoxification and activation of xenobiotics. In this study, two transcripts of Bactrocera dorsalis CPR (BdCPR) were cloned, and the deduced amino-acid sequence had an N-terminus membrane anchor for BdCPR-X1 and three conserved binding domains (FMN, FAD, and NADP), as well as an FAD binding motif and catalytic residues for both BdCPR-X1 and BdCPR-X2. BdCPR-X1 was detected to have the high expression levels in adults and in Malpighian tubules, fat bodies, and midguts of adults, but BdCPR-X2 expressed lowly in B. dorsalis. The levels of BdCPRs were similar in malathion-resistant strain compared to susceptible strain. However, injecting adults with double-stranded RNA against BdCPR significantly reduced the transcript levels of the mRNA, and knockdown of BdCPR increased adult susceptibility to malathion. Expressing complete BdCPR-X1 cDNA in Sf9 cells resulted in high activity determined by cytochrome c reduction and these cells had higher viability after exposure to malathion than control. The results suggest that BdCPR could affect the susceptibility of B. dorsalis to malathion and eukaryotic expression of BdCPR would lay a solid foundation for further investigation of P450 in B. dorsalis.
机译:NADPH细胞色素P450还原酶(CPR)对于细胞色素P450催化是必不可少的,这在异生物素的解毒和活化中很重要。在这项研究中,克隆了桔小实蝇CPR(BdCPR)的两个转录本,推导的氨基酸序列具有BdCPR-X1的N末端膜锚和三个保守的结合结构域(FMN,FAD和NADP)。作为FAD结合基序和BdCPR-X1和BdCPR-X2的催化残基。 BdCPR-X1在成年人中以及在成年人的Malpighian肾小管,脂肪体和中肠中均具有高表达水平,但BdCPR-X2在背果双歧杆菌中表达较低。与易感菌株相比,马拉硫磷抗性菌株中的BdCPRs水平相似。但是,给成年人注射针对BdCPR的双链RNA会显着降低mRNA的转录水平,而敲低BdCPR则会增加成年人对马拉硫磷的敏感性。在Sf9细胞中表达完整的BdCPR-X1 cDNA导致通过细胞色素c还原确定的高活性,并且与马拉松相比,这些细胞在暴露于马拉硫磷后具有更高的生存力。结果表明,BdCPR可能会影响背侧双歧杆菌对马拉硫磷的敏感性,而BdCPR的真核表达将为进一步研究背侧双歧杆菌中的P450奠定坚实的基础。

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