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镉对仓鼠、小鼠和大鼠卵巢的毒性作用。

Cadmium-induced ovarian toxicity in hamsters, mice, and rats.

作者信息

Rehm S, Waalkes M P

机构信息

Tumor Pathology and Pathogenesis Section, National Cancer Institute, Frederick Cancer Research Facility, Maryland 21701-1013.

出版信息

Fundam Appl Toxicol. 1988 May;10(4):635-47. doi: 10.1016/0272-0590(88)90190-x.

Abstract

The effects of cadmium on the female genital tract of Syrian hamsters (Cr:RGH), of four mouse strains (BALB/cAnNCr, DBA/2NCr, C57BL/6NCr, NFS/NCr), and two rat strains (F344/NCr and WF/NCr) were studied by light microscopy after a single sc injection of cadmium chloride (CdCl2). Experiments involved animals prior to and after sexual maturity, and employed CdCl2 doses ranging from 20 to 47.5 mumol/kg. Animals were examined at intervals from 24 hr to 8 weeks following treatment. Syrian hamsters were most susceptible to CdCl2-induced ovarian hemorrhagic necrosis at all ages tested. Most severe ovarian lesions occurred in immature hamsters, in mature hamsters at high doses, and shortly before ovulation at all doses. The small arteries of the developing follicles and interstitial stroma seemed selectively susceptible to CdCl2 toxicity while the corpora lutea, mesothelium, primordial oocytes, and the rete ovarii appeared resistant. Pretreatment with zinc acetate markedly reduced the extent of ovarian lesions in hamsters. Although reduced in weight by 45%, the hamster ovaries recovered morphologically within 2 months after severe acute hemorrhagic necrosis. Uterine and cervical stromal hemorrhages were seen only in immature hamsters at doses of greater than or equal to 30 mumol CdCl2/kg. Of the mice, only the DBA/2NCr strain showed significant CdCl2-induced ovarian hemorrhages, and these hemorrhages occurred at doses also producing lethal liver toxicity. Lesions of the uterus were rare. Rats showed dose- and age-dependent toxicity in the ovaries, uterus, cervix, and liver. CdCl2 exposure in mature rats induced uterine lesions only in F344 rats, while acute ovarian and hepatic toxicity was less severe in mature animals of both strains. No lesions were noted after 7 days in mature WF rats. In both rats and mice, no cycle dependency of the ovarian lesions was evident.

摘要

通过单次皮下注射氯化镉(CdCl₂)后,利用光学显微镜研究了镉对叙利亚仓鼠(Cr:RGH)、四种小鼠品系(BALB/cAnNCr、DBA/2NCr、C57BL/6NCr、NFS/NCr)以及两种大鼠品系(F344/NCr和WF/NCr)雌性生殖道的影响。实验涉及性成熟前后的动物,使用的CdCl₂剂量范围为20至47.5 μmol/kg。在处理后的24小时至8周内定期检查动物。在所有测试年龄中,叙利亚仓鼠对CdCl₂诱导的卵巢出血性坏死最为敏感。最严重的卵巢病变发生在未成熟仓鼠、高剂量的成熟仓鼠以及所有剂量下排卵前不久的仓鼠。发育中的卵泡和间质基质的小动脉似乎对CdCl₂毒性具有选择性易感性,而黄体、间皮、原始卵母细胞和卵巢网则表现出抗性。用醋酸锌预处理可显著降低仓鼠卵巢病变的程度。尽管仓鼠卵巢重量减轻了45%,但在严重急性出血性坏死后2个月内形态上得以恢复。仅在未成熟仓鼠中,当CdCl₂剂量大于或等于30 μmol/kg时,可见子宫和宫颈基质出血。在小鼠中,只有DBA/2NCr品系表现出显著的CdCl₂诱导的卵巢出血,且这些出血发生在也会产生致命肝毒性的剂量下。子宫病变很少见。大鼠在卵巢、子宫、宫颈和肝脏中表现出剂量和年龄依赖性毒性。成熟大鼠接触CdCl₂仅在F344大鼠中诱导子宫病变,而两种品系的成熟动物中急性卵巢和肝毒性较轻。成熟的WF大鼠在7天后未发现病变。在大鼠和小鼠中,卵巢病变均未表现出周期依赖性。

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