Faber Willem D, Deyo James A, Stump Donald G, Navarro Lisa, Ruble Karen, Knapp John
WFTC, LLC, Victor, NY 14564, USA.
Birth Defects Res B Dev Reprod Toxicol. 2007 Oct;80(5):396-405. doi: 10.1002/bdrb.20130.
These studies were conducted to evaluate the potential adverse effects of di-2-ethylhexyl terephthalate (DEHT) exposure on in utero development in mice and rats. In addition, a uterotrophic assay for estrogenic activity was conducted in sexually immature rats.
In the developmental toxicity studies, diet containing DEHT was fed to four groups of mated female Crl:CD(SD)IGS BR rats (25/group) from gestation day (GD) 0-20 or Crl:CD1(ICR) mice (25/group) from GD 0-18. Concentrations within the feed were 0, 0.3, 0.6, and 1.0% for the rats and 0, 0.1, 0.3, and 0.7% for the mice. Laparohysterectomies were carried out on the last day of exposure and the numbers of fetuses, early and late resorptions, total implantations, and corpora lutea were recorded. The fetuses were weighed, sexed, and examined for external, visceral and skeletal malformations, and developmental variations. The dose rate from dietary DEHT exposure was 0, 226, 458, and 747 mg/kg/day in the rats and 197, 592, and 1382 mg/kg/day in the mice for the control, low, mid, and high-exposure groups, respectively.
DEHT exposure did not affect clinical observations. A slight reduction in body weight gain was noted in the high-dose level rat group; the remaining groups were unaffected. At necropsy, increased liver weights were noted in the high-dose rat group and the mid- and high-dose mouse groups. Mean numbers of implantation sites and viable fetuses, mean fetal weights, and mean litter proportions of preimplantation loss, early resorptions, late resorptions, and fetal sex ratios were unaffected by DEHT exposures. No test article-related malformations or variations were observed at any concentration level in the rat and mouse developmental toxicity studies. In the uterotrophic assay for estrogenic activity, sexually immature female rats received oral gavage doses 20, 200, or 2000 mg DEHT/kg bw/day from postnatal day (PND) 19-21. A slight reduction in rate of body weight gain was noted on the first day of dosing in the high dose group, but no other indications of toxicity were evident. DEHT exposure did not affect wet or blotted uterine weight parameters in any of these dose groups. The NOEL for developmental toxicity in rats was 747 mg/kg/day and 1382 mg/kg/day in mice. The NOEL for estrogenic activity was 2000 mg/kg/day. The NOEL for maternal toxicity was 458 mg/kg/day in rats and 197 mg/kg/day in mice.
The lack of adverse developmental effects with DEHT exposure are in contrast to the adverse developmental effects noted after di-2-ethylhexyl phthalate (DEHP) exposure. The difference between the effects noted with the ortho-constituent (DEHP) and the lack of effects reported with the para-constituent (DEHT) is due most likely to differences in metabolism and the formation of the stable monoester, mono-2-ethylhexyl phthalate (MEHP) from the DEHP moiety.
开展这些研究以评估邻苯二甲酸二(2-乙基己基)酯(DEHT)暴露对小鼠和大鼠子宫内发育的潜在不良影响。此外,还对性未成熟大鼠进行了雌激素活性的子宫增重试验。
在发育毒性研究中,从妊娠第0天至第20天,给四组已交配的雌性Crl:CD(SD)IGS BR大鼠(每组25只)或从妊娠第0天至第18天,给四组Crl:CD1(ICR)小鼠(每组25只)喂食含DEHT的饲料。大鼠饲料中的浓度分别为0、0.3%、0.6%和1.0%,小鼠饲料中的浓度分别为0、0.1%、0.3%和0.7%。在暴露的最后一天进行剖腹子宫切除术,记录胎儿数量、早期和晚期吸收胎、总着床数和黄体数。对胎儿进行称重、性别鉴定,并检查其外部、内脏和骨骼畸形以及发育变异情况。大鼠对照组、低剂量组、中剂量组和高剂量组经饮食暴露于DEHT的剂量率分别为0、226、458和747 mg/kg/天,小鼠分别为197、592和1382 mg/kg/天。
DEHT暴露未影响临床观察结果。高剂量水平大鼠组体重增加略有减少;其余组未受影响。尸检时,高剂量大鼠组以及中剂量和高剂量小鼠组肝脏重量增加。着床部位和活胎的平均数量、平均胎儿体重以及着床前丢失、早期吸收胎、晚期吸收胎的平均窝比例和胎儿性别比例均不受DEHT暴露的影响。在大鼠和小鼠发育毒性研究的任何浓度水平下,均未观察到与受试物相关的畸形或变异。在雌激素活性的子宫增重试验中,性未成熟雌性大鼠从出生后第19天至第21天经口灌胃给予20、200或2000 mg DEHT/kg体重/天。高剂量组在给药第一天体重增加率略有降低,但未出现其他毒性迹象。DEHT暴露在任何这些剂量组中均未影响子宫湿重或干重参数。大鼠发育毒性的无观察到有害作用水平(NOEL)为747 mg/kg/天,小鼠为1382 mg/kg/天。雌激素活性的NOEL为2000 mg/kg/天。大鼠母体毒性的NOEL为458 mg/kg/天,小鼠为197 mg/kg/天。
DEHT暴露未产生不良发育影响,这与邻苯二甲酸二(2-乙基己基)酯(DEHP)暴露后观察到的不良发育影响形成对比。邻位成分(DEHP)所观察到的影响与对位成分(DEHT)所报告的无影响之间的差异,很可能是由于代谢差异以及从DEHP部分形成稳定的单酯单-2-乙基己基邻苯二甲酸酯(MEHP)所致。
