盐酸(-)-心得安对映体对小白鼠的抑制作用——一项安慰剂对照随机研究。

R M Kuzeff, R P Mecheva, M N Topashka-Ancheva
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引用次数: 9

摘要

背景:先前进行了一项初步研究,以观察盐酸(S)-(-)-心得安的毒性是否可以通过其对映体的增强制剂来抑制。目前的研究是基于这样的假设,即光学异构体的毒性作用可以通过施用其其中一种立体异构体,特别是对映体的增强制剂来抵消或逆转。方法:采用ICR常规小鼠508只。254只小鼠在实验前和实验中被给予(R)-(+)-心得安盐酸顺势疗法效力,另外254只小鼠被给予难以区分的安慰剂。在实验当天,小鼠腹腔注射罗美达麻醉。镇静后,小鼠腹腔注射LD50剂量的盐酸(-)-心得安。结果:统计学分析的终点是安慰剂组和治疗组小鼠的生存差异。治疗组小鼠与安慰剂组小鼠的生存优势比为1.52。等生存比例假设的卡方为5.0429(1个自由度),p值为0.0247。然后使用逻辑回归(LR)模型对小鼠体重和(-)-普萘洛尔腹腔注射剂量进行校正。LR处理优势比为1.51,LR处理卡方为4.8112(1自由度),p值为0.0283。因此,我们拒绝治疗对生存无影响的原假设。接受治疗的老鼠比服用安慰剂的老鼠多活了11%。结论:我们得出结论,在ICR常规小鼠中,腹腔注射(-)-普萘洛尔HCl的毒性可以通过给药其对映体的效价来抵消,这些小鼠在腹腔注射罗美达之前存活,并预先给药(+)-普萘洛尔HCl顺势疗法的效价。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Inhibition of (-)-propranolol hydrochloride by its enantiomer in white mice--a placebo-controlled randomized study.

Background: A previous pilot study was performed to see if toxicity of (S)-(-)-propranolol hydrochloride may be inhibited by a potentized preparation of its enantiomer. The present study is based on the hypothesis that the toxic effects of an optical isomer, may be counteracted or reversed by the administration of a potentized preparation of one of its stereoisomers, and in particular the enantiomer.

Methods: 508 ICR conventional mice were used. 254 mice were administered (R)-(+)-propranolol HCl homeopathic potency prior to and during the experiment, and the other 254 were administered indistinguishable placebo. On the day of the experiment mice were anesthetized with intraperitoneal Rometar. Once sedated the mice were administered the LD50 dose of (-)-propranolol HCl intraperitoneally.

Results: The end point for statistical analysis was the difference in survival between the placebo and treatment mice. The odds ratio for survival of treatment mice relative to placebo mice was 1.52. The hypothesis of equal survival proportions gave a chi-square of 5.0429 (1 degree of freedom), which has a p-value of 0.0247. The analysis was then adjusted for mouse weight and intraperitoneal (-)-propranolol dosage using a logistic regression (LR) model. The LR treatment odds ratio was 1.51 and the LR treatment chi-square was 4.8112 (1 degree of freedom), which has a p-value of 0.0283. Consequently, we reject the null hypothesis of no treatment effect on survival. Eleven percent more treatment mice survived than placebo mice.

Conclusion: We conclude that the toxicity of intraperitoneal (-)-propranolol HCl, may be counteracted by administration of a potency of its enantiomer, in ICR conventional mice which have survived preceding intraperitoneal Rometar injection, and pre-dosing with (+)-propranolol HCl homeopathic potency.

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