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土壤真菌弯颈霉 ATCC36112 对杀虫剂氟虫腈的代谢。

Metabolism of an insecticide fipronil by soil fungus Cunninghamella elegans ATCC36112.

机构信息

College of Plant Health and Medicine, Qingdao Agricultural University, Changcheng Rd, Chengyang, Qingdao City, 266-109, Shandong Province, China.

Department of Agricultural Biotechnology, Seoul National University, 599 Gwanak-ro, Silim-dong, Gwanak-Gu, Seoul, 151-742, Republic of Korea.

出版信息

Arch Microbiol. 2023 Jun 14;205(7):264. doi: 10.1007/s00203-023-03594-w.

Abstract

In this study, the metabolic pathway of the phenylpyrazole insecticide fipronil in Cunninghamella elegans (C. elegans) was investigated. Approximately 92% of fipronil was removed within 5 days, and seven metabolites were accumulated simultaneously. The structures of the metabolites were completely or tentatively identified by GC-MS and H, C NMR. To determine the oxidative enzymes involved in metabolism, piperonyl butoxide (PB) and methimazole (MZ) were used, and the kinetic responses of fipronil and its metabolites were determined. PB strongly inhibited fipronil metabolism, while MZ weakly inhibited its metabolism. The results suggest that cytochrome P450 (CYP) and flavin-dependent monooxygenase (FMO) may participate in fipronil metabolism. Integrated metabolic pathways can be inferred from the control and inhibitor experiments. Several novel products from the fungal transformation of fipronil were identified, and similarities between C. elegans transformation and mammalian metabolism of fipronil were compared. Therefore, these results will help to gain insight into the fungal degradation of fipronil and potential applications in fipronil bioremediation. At present, microbial degradation of fipronil is the most promising approach and maintains environmental sustainability. In addition, the ability of C. elegans to mimic mammalian metabolism will assist in illustrating the metabolic fate of fipronil in mammalian hepatocytes and assess its toxicity and potential adverse effects.

摘要

在这项研究中,研究了苯吡唑类杀虫剂氟虫腈在脉胞菌(C. elegans)中的代谢途径。大约 92%的氟虫腈在 5 天内被去除,同时同时积累了七种代谢物。通过 GC-MS 和 H、C NMR 完全或初步确定了代谢物的结构。为了确定参与代谢的氧化酶,使用了增效醚(PB)和甲巯咪唑(MZ),并测定了氟虫腈及其代谢物的动力学响应。PB 强烈抑制氟虫腈代谢,而 MZ 则弱抑制其代谢。结果表明,细胞色素 P450(CYP)和黄素依赖性单加氧酶(FMO)可能参与氟虫腈代谢。从对照和抑制剂实验可以推断出综合的代谢途径。从氟虫腈的真菌转化中鉴定出了几种新的产物,并比较了 C. elegans 转化与氟虫腈在哺乳动物体内代谢的相似性。因此,这些结果将有助于深入了解真菌对氟虫腈的降解作用以及在氟虫腈生物修复中的潜在应用。目前,微生物降解氟虫腈是最有前途的方法,并且保持了环境的可持续性。此外,C. elegans 模拟哺乳动物代谢的能力将有助于阐明氟虫腈在哺乳动物肝细胞中的代谢命运,并评估其毒性和潜在的不良影响。

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