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首页> 外文期刊>Reproductive toxicology >Developmental toxicity evaluation of triclopyr butoxyethyl ester and triclopyr triethylamine salt in the CD rat.
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Developmental toxicity evaluation of triclopyr butoxyethyl ester and triclopyr triethylamine salt in the CD rat.

机译:毛lop素丁氧基乙酯和毛lop素三乙胺盐在CD大鼠中的发育毒性评价。

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摘要

Triclopyr (3,5,6-trichloro-2-pyridyloxyacetic acid) is an herbicide used extensively in the control of woody plants and broadleaf weeds, and is often formulated as a triethylamine salt (T-TEA) or butoxyethyl ester (T-BEE). This study evaluated the developmental toxicity of T-TEA or T-BEE in time-mated CD rats gavaged on gestation days 6-15 with 0, 30, 100 or 300 mg/kg body weight(bw)/day. The doses of each compound were equimolar and equivalent to 22, 76, 216 mg/kg bw/day of triclopyr, based on prior studies indicating rapid cleavage of the salt or ester and equivalent pharmacokinetics for the active ingredient. T-TEA caused maternal toxicity, evidenced by the death of one high-dose dam, reduced body weight gain, increased relative liver and kidney weights (300 mg/kg bw/day), reduced feed consumption, and increased water consumption (100 and 300 mg/kg bw/day). Developmental effects were limited to slightly decreased fetal body weight and reduced skeletal ossification at the high dose level. T-BEE caused similar, albeit slightly more severe, maternal toxicity, with three maternal deaths at 300 mg/kg bw/day, and slight maternal effects at 30 mg/kg bw/day. Due to an equivocal increase in malformations, which were mainly clustered in litters from three high dose dams with marked maternal toxicity, the T-BEE study was repeated using 30 dams/group, investigator-blind fetal evaluations, and an additional dose group (5 mg/kg bw/day). In the repeat study, the only reproducible fetal effect was an increased incidence of 14th thoracolumbar rib at 300 mg/kg bw/day. Overall analysis of the two T-BEE studies suggested that the fetal malformations unique to the initial study likely reflected a combination of spontaneous events, exacerbated by marked maternal toxicity. The combined weight of evidence from these developmental toxicity studies, coupled with their known pharmacokinetic equivalence, indicates that T-BEE and T-TEA are not selectively toxic to the fetus. The respective maternal toxicity no-observed effect levels (NOEL) for T-BEE and T-TEA were 5 and 30 mg/kg bw/day, while the NOEL for developmental toxicity was 100 mg/kg bw/day for both compounds.
机译:Triclopyr(3,5,6-trichloro-2-pyridyloxyacetic acid)是一种除草剂,广泛用于控制木本植物和阔叶杂草,通常配制成三乙胺盐(T-TEA)或丁氧基乙酯(T-BEE )。这项研究评估了T-TEA或T-BEE在妊娠第6-15天以0、30、100或300 mg / kg体重(bw)/天的时间配对的CD大鼠中的发育毒性。根据先前的研究表明,盐或酯的快速裂解以及活性成分的等效药代动力学,每种化合物的剂量均等摩尔,相当于22、76、216 mg / kg bw /天的敌敌畏。 T-TEA引起母体毒性,表现为一个高剂量水坝死亡,体重减轻,肝脏和肾脏相对重量增加(300 mg / kg体重/天),饲料消耗减少和水消耗增加(100和300毫克/千克体重/天)。发育影响仅限于在高剂量水平下胎儿体重略有减少和骨骼骨化减少。 T-BEE引起类似的母体毒性,尽管稍重,但有3例母体死亡,每天300 mg / kg bw,而对母体的影响则为30 mg / kg bw /天。由于畸形的增加模棱两可,主要集中在三个母体毒性较大的高剂量母猪的产仔中,因此使用30个母鼠/组,研究者盲法胎儿评估和另外一个剂量组重复进行了T-BEE研究(5毫克/千克体重/天)。在重复研究中,唯一可重现的胎儿效应是第300毫克/千克体重/天的第14胸腰大肋骨发生率增加。两项T-BEE研究的整体分析表明,最初研究所独有的胎儿畸形可能反映了自发事件的组合,并伴随着明显的母体毒性。这些发育毒性研究的证据总重量加上其已知的药代动力学等效性,表明T-BEE和T-TEA对胎儿没有选择性毒性。孕妇对T-BEE和T-TEA的未观察到的毒性水平(NOEL)分别为5和30 mg / kg bw /天,而两种化合物对发育毒性的NOEL均为100 mg / kg bw /天。

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