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普拉米维林的毒理学研究(作者译)

[Toxicological study on pramiverine (author's transl)].

作者信息

Eberstein M, Frohberg H, Hofmann A, Jochmann G, Metallinos A, Schiling B, Weisse G

出版信息

Arzneimittelforschung. 1976 Apr;26(4b):703-9.

PMID:989019
Abstract

4,4-Diphenyl-N-isopropyl-cyclohexylamine-hydrochloride (pramiverine, Sistalgin) was investigated alone and in combination (1 + 1000) with N-methyl-N-(2,3-dimethyl-5-oxo-1-phenyl-3-pyrazolin-4-yl)-aminomethanesulfonate (metamizole) in various species for acute toxicity after oral and intravenous administration, for local tolerance and subacute toxicity. In addition, long-term trials and reproduction toxicity studies were performed with pramiverine. Pramiverine was only slightly toxic and was well tolerated locally as an ampoule solution also in combination with metamizole. The acute trials of the two compounds in mice and rats like the subacute study in rats showed that the toxicity of metamizole was not increased by pramiverine. Rats tolerated in the long-term trial all pramiverine doses examined (0.5; 5.0; 50.0 mg/kg), while cholinolytic concomitant effects were observed in dogs under higher doses (5.0 and 20.0 mg/kg). Pramiverine did not have a foetotoxic and teratogenic effect in mice, rats and rabbits. In the perinatal and postnatal experiment in rats no effect on foetal development, viability and growth of the offspring as well as the course of labour and lactation ability of the dams was observed.

摘要

对4,4-二苯基-N-异丙基-环己胺盐酸盐(普拉米维林,西斯塔金)单独以及与N-甲基-N-(2,3-二甲基-5-氧代-1-苯基-3-吡唑啉-4-基)氨基甲磺酸盐(安乃近)按1 + 1000的比例联合使用,在多种动物中进行了口服和静脉给药后的急性毒性、局部耐受性和亚急性毒性研究。此外,还对普拉米维林进行了长期试验和生殖毒性研究。普拉米维林毒性轻微,作为安瓿溶液局部耐受性良好,与安乃近联合使用时也是如此。两种化合物在小鼠和大鼠中的急性试验以及在大鼠中的亚急性研究表明,普拉米维林不会增加安乃近的毒性。在长期试验中,大鼠耐受所有测试的普拉米维林剂量(0.5;5.0;50.0 mg/kg),而在较高剂量(5.0和20.0 mg/kg)下,犬出现了抗胆碱能伴随效应。普拉米维林对小鼠、大鼠和兔子没有胚胎毒性和致畸作用。在大鼠的围产期和产后实验中,未观察到对胎儿发育、后代活力和生长以及母鼠分娩过程和泌乳能力的影响。

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