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长期暴露于八甲基环四硅氧烷和十甲基环五硅氧烷对老年雌性费希尔344大鼠的影响。

Effects of chronic exposure to octamethylcyclotetrasiloxane and decamethylcyclopentasiloxane in the aging female Fischer 344 rat.

作者信息

Jean Paul A, Sloter Eddie D, Plotzke Kathleen P

机构信息

Dow Corning Corporation, Midland, MI, 48686, United States.

Charles River Laboratories International, Inc, United States.

出版信息

Toxicol Lett. 2017 Oct 20;279 Suppl 1:54-74. doi: 10.1016/j.toxlet.2017.08.016. Epub 2017 Aug 23.

DOI:10.1016/j.toxlet.2017.08.016
PMID:28842205
Abstract

Octamethylcyclotetrasiloxane (D4) and decamethylcyclopentasiloxane (D5) are used as intermediates or monomers in the synthesis of silicon-based polymers for industrial or consumer applications. D4 and D5 may remain as residual monomer in these polymers at less than 1000ppm and may therefore be present as a minor impurity in consumer products. For D5, in addition to the manufacture of polymers, its uses include intentional addition to consumer products, personal care products and some dry- cleaning solvents. Two-year rodent chronic bioassays were conducted with both substances and borderline increases in the incidence of uterine tumors were observed, specifically, benign uterine adenoma with D4 and adenocarcinoma with D5. The effects profile and induction of uterine tumors share some similarity with that seen with chronic exposure to dopamine agonists. The current study investigated the potential for D4 and D5 to elicit dopamine agonist-like effects on estrous cyclicity. Separate groups of reproductively senescent female Fischer 344 rats (F344) were exposed via vapor inhalation to D4 (700ppm, 9.3mg/L) or D5 (160ppm, 2.1mg/L) or to a diet containing 0.0045, 0.045, or 4.5ppm pergolide mesylate (PM), a potent dopamine agonist used here as a reference substance, from 11 through 24 months of age. The primary focus was to characterize the effects of D4 and D5 exposure on estrous cyclicity relative to that observed with PM. As a monitoring effort, circulating endogenous estradiol, progesterone, prolactin and corticosterone levels were evaluated monthly. A blood sample from each rat was obtained via tail vein in the afternoon after the daily inhalation exposure period once every 4 weeks. Histomorphologic examination of the major organs including the reproductive tract was conducted on all animals at study termination. This study has shown that chronic exposure to D4 and D5 can affect cyclicity in the reproductively senescent F344 rat. For each substance the effect on cyclicity involved reduction in the incidence of pseudopregnancy with a shift toward cycles more typical of younger animals. D4 and D5 induced an increase in estrous cycle repetition whereas D4 also increased the incidence of extended estrus. These shifts resulted in animals entering proestrus/estrus significantly more times over the duration of the study than seen in the control group. Similar effects were observed with the reference substance, PM. However, distinct differences in the timing and magnitude of the effects on the estrous cycle and impact on prolactin, progesterone, estradiol, and corticosterone suggest that D4 and D5 are not classical dopamine agonists even though a similar increased incidence of proestrus/estrus was also observed with PM. These results may prove important with respect to understanding D4- and D5-induced uterine tumor response in the F344 rat, given the relationship between increased incidence of uterine endometrium stimulation by endogenous estrogen as a consequence of extended or more frequent proestrus/estrus, uterine tumor risk, and questions of relevance to humans. Recent publications have summarized the existing data on D4 and D5, with emphasis on exploring the biological relevance of the uterine tumors (Klaunig et al., 2016a,b; Franzen et al., 2017; Dekant and Klaunig, 2016; Dekant et al., 2017). The authors concluded that although the mode of action has not yet been fully established, the data, including the findings from this study, indicate that the D4- and D5-induced uterine tumors observed in the rodent chronic bioassays have no relevance for human risk characterization based not only on the distinct species differences in regulation of the reproductive systems, but also the high exposure levels and duration required for expression in rats.

摘要

八甲基环四硅氧烷(D4)和十甲基环五硅氧烷(D5)在用于工业或消费应用的硅基聚合物合成中用作中间体或单体。D4和D5在这些聚合物中可能以残留单体形式存在,含量低于1000ppm,因此可能作为微量杂质存在于消费品中。对于D5,除了用于聚合物制造外,其用途还包括有意添加到消费品、个人护理产品和一些干洗溶剂中。对这两种物质都进行了为期两年的啮齿动物慢性生物测定,观察到子宫肿瘤发生率有临界性增加,具体而言,D4导致良性子宫腺瘤,D5导致腺癌。其效应特征和子宫肿瘤的诱发与长期接触多巴胺激动剂有一些相似之处。本研究调查了D4和D5对动情周期产生类似多巴胺激动剂效应的可能性。将处于生殖衰老期的雌性Fischer 344大鼠(F344)分成不同组,从11月龄到24月龄,通过蒸汽吸入暴露于D4(700ppm,9.3mg/L)或D5(160ppm,2.1mg/L),或暴露于含有0.0045、0.045或4.5ppm甲磺酸培高利特(PM)的饲料中,PM是一种强效多巴胺激动剂,在此用作参考物质。主要重点是相对于PM所观察到的情况,表征D4和D5暴露对动情周期的影响。作为一项监测工作,每月评估循环中的内源性雌二醇、孕酮、催乳素和皮质酮水平。在每天吸入暴露期后的下午,每4周通过尾静脉从每只大鼠采集一次血样。在研究结束时,对所有动物包括生殖道在内的主要器官进行组织形态学检查。本研究表明,长期暴露于D4和D5会影响生殖衰老期F344大鼠的动情周期。对于每种物质,对动情周期的影响包括假孕发生率降低,且向更典型的年轻动物周期转变。D4和D使动情周期重复次数增加,而D4还增加了发情期延长的发生率。这些转变导致动物在研究期间进入动情前期/发情期的次数明显多于对照组。参考物质PM也观察到类似效应。然而,对动情周期的影响在时间和程度上以及对催乳素、孕酮、雌二醇和皮质酮的影响存在明显差异,这表明D4和D5不是经典的多巴胺激动剂,尽管PM也观察到类似的动情前期/发情期发生率增加。鉴于延长或更频繁的动情前期/发情期导致内源性雌激素对子宫内膜刺激增加、子宫肿瘤风险以及与人类相关性的问题之间的关系,这些结果对于理解F344大鼠中D4和D5诱导的子宫肿瘤反应可能具有重要意义。最近的出版物总结了关于D4和D5的现有数据,重点是探索子宫肿瘤的生物学相关性(Klaunig等人,2016a、b;Franzen等人,2017;Dekant和Klaunig,2016;Dekant等人,2017)。作者得出结论,尽管作用模式尚未完全确立,但包括本研究结果在内的数据表明,在啮齿动物慢性生物测定中观察到的D4和D5诱导的子宫肿瘤与人类风险评估无关,这不仅基于生殖系统调节方面明显的物种差异,还基于大鼠中表达所需的高暴露水平和持续时间。

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