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与褐飞虱对啶虫脒抗性相关的代谢解毒作用和靶标位点突变

Metabolic detoxification and target site mutations associated with acetamiprid resistance in L.

作者信息

Samal Roopa Rani, Panmei Kungreiliu, Lanbiliu P, Kumar Sarita

机构信息

Department of Zoology, Acharya Narendra Dev College, University of Delhi, New Delhi, India.

出版信息

Front Physiol. 2022 Aug 30;13:988907. doi: 10.3389/fphys.2022.988907. eCollection 2022.

Abstract

Despite the continuous use of chemical interventions, -borne diseases remain on the rise. Neonicotinoids are new, safer, and relatively effective pharmacological interventions against mosquitoes. Neonicotinoids interact with the postsynaptic nicotinic acetylcholine receptors (nAChRs) of the insect central nervous system, but the absence of nAChR polymorphism in resistant phenotypes makes their involvement in neonicotinoid resistance uncertain. Thus, an investigation was carried out to understand the role of metabolic detoxification and target site insensitivity in imparting acetamiprid resistance in larvae. Studies were conducted on the parent susceptible strain (PS), acetamiprid-larval selected strain for five generations (ACSF-5; 8.83-fold resistance) and 10 generations (ACSF-10; 19.74-fold resistance) of . The larval selection raised α-esterase and β-esterase activities by 1.32-fold and 1.34-fold, respectively, in ACSF-10 as compared to PS, while the corresponding glutathione-S-transferase and acetylcholinesterase activity increased by 22.5 and 2%. The gene in PS and ACSF-10 showed four mismatches in the 1312-1511 bp region due to mutations in the Y455C codon (tyrosine to cysteine) at the 1367th position (TAC→TGC); I457V codon (isoleucine to valine) at 1372 bp and 1374 bp (ATA→GTG); and R494M codon (arginine to methionine) at 1484 bp (AGG→ATG). The R494M mutation was the novel and dominant type, observed in 70% ACSF-10 population, and has not been reported so far. The studies evidenced the combination of metabolic detoxification and target site mutation in imparting acetamiprid resistance in .

摘要

尽管持续使用化学干预措施,但虫媒疾病仍在增加。新烟碱类是针对蚊子的新型、更安全且相对有效的药物干预措施。新烟碱类与昆虫中枢神经系统的突触后烟碱型乙酰胆碱受体(nAChRs)相互作用,但抗性表型中缺乏nAChR多态性使得它们在新烟碱类抗性中的作用尚不确定。因此,开展了一项研究以了解代谢解毒和靶标位点不敏感性在赋予淡色库蚊对啶虫脒抗性中的作用。对亲本敏感品系(PS)、经五代啶虫脒幼虫选育的品系(ACSF - 5;抗性为8.83倍)和十代选育的品系(ACSF - 10;抗性为19.74倍)的淡色库蚊进行了研究。与PS相比,在ACSF - 10中,幼虫选育使α - 酯酶和β - 酯酶活性分别提高了1.32倍和1.34倍,而相应的谷胱甘肽 - S - 转移酶和乙酰胆碱酯酶活性分别增加了22.5%和2%。PS和ACSF - 10中的基因在1312 - 1511 bp区域显示出四个错配,这是由于第1367位(TAC→TGC)的Y455C密码子(酪氨酸突变为半胱氨酸)、1372 bp和1374 bp处(ATA→GTG)的I457V密码子(异亮氨酸突变为缬氨酸)以及1484 bp处(AGG→ATG)的R494M密码子(精氨酸突变为甲硫氨酸)发生突变所致。R494M突变是新出现的优势类型,在70%的ACSF - 10群体中观察到,迄今尚未见报道。这些研究证明了代谢解毒和靶标位点突变相结合赋予淡色库蚊对啶虫脒的抗性。

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