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福培特诱导的小鼠十二指肠短期细胞毒性和增殖变化。

Folpet-induced short term cytotoxic and proliferative changes in the mouse duodenum.

机构信息

Elliot Gordon Consulting, LLC, Princeton Junction, NJ, USA.

出版信息

Toxicol Mech Methods. 2012 Jan;22(1):54-9. doi: 10.3109/15376516.2011.593054. Epub 2011 Oct 21.

Abstract

Folpet, an agricultural fungicide, induces tumors in the mouse gastrointestinal tract, primarily in the duodenum. Bioassays show a threshold for tumors at ~1000 ppm dietary administration. We investigated the early histologic changes to the mouse duodenum in mice fed a diet containing 6000 ppm folpet for 28 days. Reversibility of folpet-induced changes was evaluated after treatment for 28 days and a recovery period of 17 days. Macroscopic changes in the cecum (dilatation) and duodenum (roughening) were evident by day 7, continued through day 28, then returned to normal by recovery day 17. The duodenal mucosa also appeared to be thickened. Macroscopic changes to the forestomach were also evident as a rough surface or depressions; they also decreased in incidence and severity in the recovery animals. Histologic changes of the duodenum (crypt cell hyperplasia, villous hypertrophy, numerous intraepithelial lymphocytes, and elongation of epithelial columnar cells) were evident in all treated mice by day 7 and continued and increased in severity through 28 days of administration. The incidence and severity of these findings was reduced on recovery day 17, indicating reversibility. Histologic changes (epithelial hyperplasia and hyperkeratosis) of the non-glandular squamous epithelium in the forestomach occurred later than the changes to the duodenum. The incidence and severity of these changes also lessened by recovery day 17. These early histologic changes support a non-DNA reactive mode of action for folpet carcinogenicity in mice involving the key events of mucosal cytotoxicity with consequent regenerative proliferation. Exposures that are not sufficient to produce cytotoxicity would also not lead to tumor formation.

摘要

福培,一种农业杀菌剂,会在老鼠的胃肠道中引发肿瘤,主要发生在十二指肠。生物测定显示,在饮食中摄入约 1000ppm 的福培时会产生肿瘤。我们研究了喂食含 6000ppm 福培饮食 28 天后老鼠十二指肠的早期组织学变化。在治疗 28 天后和恢复期 17 天评估了福培诱导变化的可逆性。第 7 天就已经可以观察到盲肠(扩张)和十二指肠(粗糙)的明显宏观变化,并持续到第 28 天,然后在恢复期第 17 天恢复正常。十二指肠黏膜似乎也增厚了。前胃的宏观变化也表现为表面粗糙或凹陷;在恢复期动物中,这些变化的发生率和严重程度也降低了。第 7 天所有接受治疗的老鼠的十二指肠(隐窝细胞增生、绒毛肥大、大量上皮内淋巴细胞和上皮柱状细胞伸长)均出现组织学变化,并在 28 天的给药期间持续且加重。在恢复期第 17 天,这些发现的发生率和严重程度降低,表明具有可逆性。前胃非腺状鳞状上皮的组织学变化(上皮增生和过度角化)比十二指肠晚发生。在恢复期第 17 天,这些变化的发生率和严重程度也减轻了。这些早期组织学变化支持福培在老鼠中的致癌作用是一种非 DNA 反应模式,涉及粘膜细胞毒性的关键事件,继而导致再生性增殖。不足以产生细胞毒性的暴露也不会导致肿瘤形成。

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