酚酞(CAS No. 77-09-8)在转基因单倍不足p16(Ink4a)/p19(Arf)小鼠(饲料研究)中的毒理学和致癌作用研究。

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引用次数: 0

摘要

未标注:在20世纪的大部分时间里,酚酞被普遍用作泻药。自1997年美国食品和药物管理局(FDA)提议撤销其作为非处方药的分类(21 CFR, Part 310)以来,在泻药中使用酚酞的情况有所减少。此前,美国国家毒理学计划(1996年)在为期两年的致癌性研究中对酚酞进行了评估。人类接触酚酞的主要途径是通过摄入、皮肤接触和吸入制造该化合物的工艺装置产生的污染空气。在这项研究中,酚酞的致癌作用在单倍不足p16(Ink4a)/p19(Arf)小鼠模型中进行了研究,作为NTP的持续目标是寻求毒理学和致癌研究的模型系统,特别是那些可以提供与理解药物作用方式相关的机制信息的模型系统。雄性和雌性单倍不足p16(Ink4a)/p19(Arf)小鼠暴露于饲料中的酚酞(纯度大于97%)27周。对小鼠外周血红细胞进行了遗传毒理学研究。小鼠27周研究:每组15只雄性和15只雌性小鼠暴露于0、200、375、750、3000或12000 ppm的酚酞(相当于平均每日剂量约为35、65、135、540和2170毫克/公斤体重的雄性和50、90、170、680、2770毫克/公斤体重的雌性)饲料中27周。所有暴露组雄性和雌性小鼠的存活率与对照组相似。在第11周后,12,000 ppm组的雄性平均体重低于对照组。暴露组和对照组之间的饲料消耗量没有差异。不典型胸腺增生,化学诱导的胸腺淋巴瘤的癌前病变,发生在暴露的男性和女性中,在12000 ppm的女性中发病率显著增加。睾丸精小管萎缩、睾丸间质细胞增生和附睾低精子症发生在大多数浓度为3000 ppm和12000 ppm的男性。此外,在ppm含量为3000 ppm和12000 ppm的雄性中,左、右睾丸重量、左附睾重量、精子活动力、每睾丸精细胞头数、每尾精子头数和每克附睾尾精子头数均显著低于对照组。肾病的发病率在3000 ppm和12000 ppm的男性中显著增加;接受750ppm或更高剂量的男性肾小管肥大的发生率显著增加。在所有12,000 ppm的男性中都发生了脾脏造血细胞增殖,而在375、750和12,000 ppm的女性中,这种病变的发生率显著增加。遗传毒理学:在27周的研究中,在雄性和雌性单倍体不足p16(Ink4a)/p19(Arf)小鼠的四个时间点评估微核红细胞的频率。在雄性和雌性小鼠的所有时间点都观察到微核细胞的显著浓度相关增加。结论:在为期27周的饲料研究条件下,暴露于200、375、750、3,000或12,000 ppm的雄性或雌性单倍不足p16(Ink4a)/p19(Arf)小鼠中,没有证据表明酚酞具有致癌活性。由于这是一种新模型,因此尚不确定该研究是否具有足够的灵敏度来检测致癌效应。酚酞诱导雄性和雌性小鼠胸腺的非典型增生(肿瘤前病变),雄性和雌性小鼠脾脏的造血细胞增殖,以及雄性小鼠肾脏和生殖系统的毒性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The toxicology and carcinogenesis study of phenolphthalein (CAS No. 77-09-8) in genetically modified haploinsufficient p16(Ink4a)/p19(Arf) mice (feed study).

Unlabelled: Phenolphthalein was commonly used as a laxative for most of the 20th century. The use of phenolphthalein in laxatives has decreased since 1997 when the United States Food and Drug Administration (FDA) proposed to withdraw its classification as an over-the-counter drug (21 CFR, Part 310). Phenolphthalein has been previously evaluated in 2-year carcinogenicity studies by the National Toxicology Program (1996). The major route of human exposure to phenolphthalein is via ingestion, dermal contact, and inhalation of contaminated air originating from process units manufacturing the compound. In this study, the carcinogenic effects of phenolphthalein were studied in the haploinsufficient p16(Ink4a)/p19(Arf) mouse model as an ongoing goal of the NTP is to seek model systems for toxicology and carcinogenesis studies, especially those that can provide mechanistic information relative to understanding an agent's mode of action. Male and female haploinsufficient p16(Ink4a)/p19(Arf) mice were exposed to phenolphthalein (greater than 97% pure) in feed for 27 weeks. Genetic toxicology studies were conducted in mouse peripheral blood erythrocytes. 27-WEEK STUDY IN MICE: Groups of 15 male and 15 female mice were exposed to 0, 200, 375, 750, 3,000, or 12,000 ppm phenolphthalein (equivalent to average daily doses of approximately 35, 65, 135, 540, and 2,170 mg phenolphthalein/kg body weight to males and 50, 90, 170, 680, 2,770 mg/kg to females) in feed for 27 weeks. Survival of all exposed groups of male and female mice was similar to that of the control groups. Mean body weights of males in the 12,000 ppm group were less than those of the control group after week 11. No differences in feed consumption were noted between exposed and control groups. Atypical hyperplasia of the thymus, a premalignant change of chemically induced thymic lymphoma, occurred in exposed males and females, and the incidence was significantly increased in 12,000 ppm females. Atrophy of the seminiferous tubules in the testis, hyperplasia of the testicular interstitial (Leydig) cells, and epididymal hypospermia occurred in most 3,000 and 12,000 ppm males. Additionally, the left and right testis weights, the left epididymis weights, sperm motility, the numbers of spermatid heads per testis, and sperm heads per cauda and per gram cauda epididymis were generally significantly less in 3,000 and 12,000 ppm males than in the control group. The incidences of nephropathy were significantly increased in 3,000 and 12,000 ppm males; incidences of hypertrophy of renal tubules were significantly increased in males receiving 750 ppm or greater. Hematopoietic cell proliferation of the spleen occurred in all 12,000 ppm males, and the incidences of this lesion were significantly increased in 375, 750, and 12,000 ppm females.

Genetic toxicology: The frequency of micronucleated erythrocytes was assessed at four time points during the 27-week study in male and female haploinsufficient p16(Ink4a)/p19(Arf) mice. Significant concentration-related increases in micronucleated cells were observed at all time points in male and female mice.

Conclusions: Under the conditions of this 27-week feed study, there was no evidence of carcinogenic activity of phenolphthalein in male or female haploinsufficient p16(Ink4a)/p19(Arf) mice exposed to 200, 375, 750, 3,000, or 12,000 ppm. Because this is a new model, there is uncertainty whether the study possessed sufficient sensitivity to detect a carcinogenic effect. Phenolphthalein induced atypical hyperplasia, a preneoplastic lesion of the thymus, in male and female mice, hematopoietic cell proliferation of the spleen in male and female mice, and toxicity to the kidney and reproductive system in male mice.

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