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大鼠体内丙烯酰胺及其环氧代谢产物缩水甘油酰胺的神经毒性和生殖毒性的比较研究。

Comparative studies on the neuro- and reproductive toxicity of acrylamide and its epoxide metabolite glycidamide in the rat.

作者信息

Costa L G, Deng H, Gregotti C, Manzo L, Faustman E M, Bergmark E, Calleman C J

机构信息

Department of Environmental Health, University of Washington, Seattle 98195.

出版信息

Neurotoxicology. 1992 Spring;13(1):219-24.

PMID:1508423
Abstract

The neurotoxicity of acrylamide (AA) has been the subject of extensive studies at the morphological and functional levels in both animals and man. The concern for human exposure to monomeric AA derives partly from its extensive use in molecular biology laboratories where, in the United States alone, 100,000-200,000 persons are potentially exposed. Initial work in this laboratory aiming at the development of techniques for using hemoglobin adducts as biomarkers for human exposure to AA, revealed the formation of glycidamide as a reactive epoxide metabolite of acrylamide in the rat (Chem. Res. Toxicol. 3, 406, 1990). In rats treated with 0-100 mg/kg of AA significant dose-rate effects were observed on adduct formation by both AA and glycidamide. The high rate of formation of the metabolite, especially at low doses where approximately 60% of AA was converted to glycidamide in vivo, prompted us to investigate its potential role in the induction of neurotoxic and reproductive effects attributed to AA exposure. In initial neurotoxicological experiments, the effects of the parent compound (8-14 days, 25 and 50 mg/kg/day) and the metabolite (8-14 days, 50 and 100 mg/kg/day) were compared. While at the higher dose both compounds affected the rats' performance on the rotarod, only acrylamide had a significant effect in the hindlimb splay test, which is considered a more sensitive indicator of peripheral neuropathy. On the other hand, a stronger effect was seen for glycidamide than for AA on the male reproductive system, especially on sperm cell viability.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

丙烯酰胺(AA)的神经毒性已在动物和人类的形态学和功能水平上进行了广泛研究。人们对人类接触单体AA的担忧部分源于其在分子生物学实验室中的广泛使用,仅在美国,就有10万至20万人可能接触到它。本实验室最初致力于开发利用血红蛋白加合物作为人类接触AA生物标志物的技术,结果显示在大鼠体内,环氧丙酰胺作为丙烯酰胺的一种活性环氧化物代谢产物形成(《化学研究毒理学》第3卷,第406页,1990年)。在用0至100 mg/kg AA处理的大鼠中,观察到AA和环氧丙酰胺在加合物形成上存在显著的剂量率效应。该代谢产物的高形成率,尤其是在低剂量情况下(体内约60%的AA转化为环氧丙酰胺),促使我们研究其在由AA暴露引起的神经毒性和生殖效应诱导中的潜在作用。在最初的神经毒理学实验中,比较了母体化合物(8至14天,25和50 mg/kg/天)和代谢产物(8至14天,50和100 mg/kg/天)的作用。虽然在较高剂量下两种化合物都影响大鼠在旋转棒上的表现,但只有丙烯酰胺在后肢张展试验中有显著影响,而后肢张展试验被认为是周围神经病变更敏感的指标。另一方面,环氧丙酰胺对雄性生殖系统的影响比AA更强,尤其是对精子细胞活力的影响。(摘要截选至250词)

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