The Effects of Perinatal/Juvenile Methoxychlor Exposure on Adult Rat Nervous, Immune, and Reproductive System Function

R.E. Chapin , M.W. Harris , B.J. Davis , S.M. Ward , R.E. Wilson , M.A. Mauney , A.C. Lockhart , R.J. Smialowicz , V.C. Moser , L.T. Burka , B.J. Collins
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Abstract

In order to address data gaps identified by the NAS reportPesticides in the Diets of Infants and Children,a study was performed using methoxychlor (MXC). Female rats were gavaged with MXC at 0, 5, 50, or 150 mg/kg/day for the week before and the week after birth, whereupon the pups were directly dosed with MXC from postnatal day (pnd) 7. Some dams were killed pnd7 and milk and plasma were assayed for MXC and metabolites. For one cohort of juveniles, treatment stopped at pnd21; a modified functional observational battery was used to assess neurobehavioral changes. Other cohorts of juveniles were dosed until pnd42 and evaluated for changes to the immune system and for reproductive toxicity. Dose-dependent amounts of MXC and metabolites were present in milk and plasma of dams and pups. The high dose of MXC reduced litter size by ≈17%. Ano-genital distance was unchanged, although vaginal opening was accelerated inalltreated groups, and male prepuce separation was delayed at the middle and high doses by 8 and 34 days, respectively. In the neurobehavioral evaluation, high-dose males were more excitable, but other changes were inconsistent and insubstantial. A decrease in the antibody plaque-forming cell response was seen in males only. Adult estrous cyclicity was disrupted at 50 and 150MXC, doses which also showed reduced rates of pregnancy and delivery. Uterine weights (corrected for pregnancy) were reduced in all treated pregnant females. High-dose males impregnated fewer untreated females; epididymal sperm count and testis weight were reduced at the high, or top two, doses, respectively. All groups of treated females showed uterine dysplasias and less mammary alveolar development; estrous levels of follicle stimulating hormone were lower in all treated groups, and estrus progesterone levels were lower at 50 and 150 MXC, attributed to fewer corpora lutea secondary to ovulation defects. These data collectively show that the primary adult effects of early exposure to MXC are reproductive, show that 5 mg/kg/day is not a NO(A)EL in rats with this exposure paradigm (based on changes in day of vaginal opening, pubertal ovary weights, adult uterine and seminal vesicle weights, and female hormone data) and imply that the sites of action are both central and peripheral.

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围产期/幼期甲氧氯暴露对成年大鼠神经、免疫和生殖系统功能的影响
为了解决美国国家科学院报告《婴幼儿饮食中的农药》中发现的数据缺口,使用甲氧氯(MXC)进行了一项研究。雌性大鼠在出生前一周和出生后一周分别以0、5、50、150 mg/kg/天的剂量灌胃MXC,幼鼠从出生后第7天起直接灌胃MXC。处死部分奶牛,检测乳汁和血浆中MXC及其代谢物。对于一组青少年,治疗在pnd21时停止;改良的功能观察电池用于评估神经行为变化。其他组的幼鱼被给药至pnd42,并评估免疫系统的变化和生殖毒性。MXC及其代谢物存在于母鼠和幼崽的乳和血浆中,呈剂量依赖性。高剂量MXC可使产仔数减少约17%。尽管在所有治疗组中阴道开口加速,但肛门与生殖器的距离没有变化,并且在中剂量和高剂量组中,雄性包皮分离分别延迟了8天和34天。在神经行为评估中,高剂量的雄性更容易兴奋,但其他变化不一致且不明显。抗体斑块形成细胞反应的减少只在男性中出现。在50和150MXC的剂量下,成虫的发情周期被打乱,这也显示出怀孕和分娩率的降低。所有接受治疗的孕妇子宫重量(经妊娠校正)均有所减轻。高剂量雄鼠使未经治疗的雌鼠受孕的数量较少;在高剂量或前两种剂量下,附睾精子数量和睾丸重量分别减少。所有治疗组女性均出现子宫发育不良和乳腺泡发育减少;在所有治疗组中,促卵泡激素的发情水平都较低,在50和150 MXC时,发情黄体酮水平较低,这是由于排卵缺陷继发的黄体较少。这些数据共同表明,早期暴露于MXC对成年的主要影响是生殖方面的,表明在这种暴露模式下(基于阴道开口天数、青春期卵巢重量、成年子宫和精囊重量以及雌性激素数据的变化),5mg /kg/天对大鼠的NO(a) EL没有影响,并暗示作用部位包括中枢和外周。
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