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一种评估米索硝唑对大鼠神经毒性作用的生化方法。

A biochemical method for assessing the neurotoxic effects of misonidazole in the rat.

作者信息

Rose G P, Dewar A J, Stratford I J

出版信息

Br J Cancer. 1980 Dec;42(6):890-9. doi: 10.1038/bjc.1980.337.

Abstract

A proven biochemical method for assessing chemically induced neurotoxicity has been applied to the study of the toxic effects of misonidazole (MISO) in the rat. This involves the fluorimetric measurement of beta-glucuronidase and beta-galactosidase activities in homogenates of rat nervous tissue. The tissues analysed were sciatic/posterior tibial nerve (SPTN) cut into 4 sections, trigeminal ganglia and cerebellum. MISO administered i.p. to Wistar rats in doses greater than 300 mg/kg/day for 7 consecutive days produced maximal increases in both beta-glucuronidase and beta-galactosidase activities in th SPTN at 4 weeks (140-180% of control values). The highest increases were associated with the most distal secretion of the nerve. Significant enzyme-activity changes were also found in the trigeminal ganglia and cerebellum of MISO-dosed rats. The greatest activity occurred 4-5 weeks after dosing, and was dose-related. It is concluded that, in the rat, MISO can produce biochemical changes consistent with a dying-back peripheral neuropathy, and biochemical changes suggestive of cerebellar damage. This biochemical approach would appear to offer a convenient quantitative method for the detection of neurotoxic effects of other potential radio-sensitizing drugs.

摘要

一种已被证实的评估化学诱导神经毒性的生化方法已应用于研究米索硝唑(MISO)对大鼠的毒性作用。这涉及对大鼠神经组织匀浆中β-葡萄糖醛酸酶和β-半乳糖苷酶活性进行荧光测定。所分析的组织是切成4段的坐骨/胫后神经(SPTN)、三叉神经节和小脑。以大于300mg/kg/天的剂量连续7天腹腔注射给Wistar大鼠的MISO,在4周时使SPTN中的β-葡萄糖醛酸酶和β-半乳糖苷酶活性均出现最大程度增加(为对照值的140 - 180%)。最高的增加与神经最远端部分相关。在给予MISO的大鼠的三叉神经节和小脑中也发现了显著的酶活性变化。最大活性出现在给药后4 - 5周,且与剂量相关。得出的结论是,在大鼠中,MISO可产生与逆行性周围神经病变一致的生化变化以及提示小脑损伤的生化变化。这种生化方法似乎为检测其他潜在放射增敏药物的神经毒性作用提供了一种便捷的定量方法。

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