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A detailed study of developmental immunotoxicity of imidacloprid in Wistar rats.

机译:吡虫啉对Wistar大鼠发育免疫毒性的详细研究。

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Human exposure to imidacloprid is likely to occur during its use as an acaricide or an ectoparasiticide. Accordingly, the developmental immunotoxic potential of imidacloprid was investigated. Oral exposure was initiated in timed pregnant female Wistar rats on gestation day 6 (GD 6) till GD 21. On GD 20, half of the gravid dams were sacrificed, and in utero fetal development was assessed. In the other half of the dams, administration was continued till weaning on postnatal day 21 (PND 21) and maternal toxicity was investigated. A subgroup of weaned pups was sacrificed to assess immunotoxicity parameters. The other half of the pups were exposed to imidacloprid till PND 42, and immunotoxicity was assessed. The findings revealed post-implantation loss in the highest dose group, indicating the risk of abortion. Soft tissue abnormalities and skeletal alterations were observed in the highest dose group. Humoral immunity was assessed by estimating hemagglutination titer and immunoglobulin production. Cell mediated immunity was assessed by Delayed Type Hypersensitivity, whereas, non-specific immunity was assessed by phagocytic index, and other phenotypic parameters. These data revealed that imidacloprid caused age-dependent adverse effects on the developing immunity which was aggravated when exposure continued throughout development, leading to a compromised immune system.
机译:人体将吡虫啉用作杀螨剂或杀螨剂的过程中很容易发生。因此,研究了吡虫啉的发展性免疫毒性潜力。在妊娠第6天(GD 6)至GD 21开始在定时怀孕的雌性Wistar大鼠中开始口服暴露。直到GD21。在GD 20时,牺牲了一半的妊娠水坝,并评估了子宫内胎儿的发育。在水坝的另一半,继续给药直至出生后第21天(PND 21)断奶,并调查了母体毒性。处死断奶仔猪亚组以评估免疫毒性参数。将另一半幼犬暴露于吡虫啉直至PND 42,并评估免疫毒性。研究结果显示最高剂量组的植入后损失,表明存在流产的风险。在最高剂量组中观察到软组织异常和骨骼改变。通过估计血凝滴度和免疫球蛋白产生来评估体液免疫。通过迟发型超敏反应评估细胞介导的免疫,而通过吞噬指数和其他表型参数评估非特异性免疫。这些数据表明吡虫啉对发育中的免疫力产生年龄依赖性的不利影响,在整个发育过程中持续暴露会加剧这种不良反应,导致免疫系统受损。

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