金不换与雪上一枝蒿不同比例配伍的减毒增效作用

李梅; 陈慧; 柯才华; 黄先菊

doi:10.13422/j.cnki.syfjx.2018030166

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金不换与雪上一枝蒿不同比例配伍的减毒增效作用

毒理 | 更新时间：2024-01-04

- 金不换与雪上一枝蒿不同比例配伍的减毒增效作用
- Decreasing Toxicity and Increasing Efficacy Through Different Compatibilities of and
- 中国实验方剂学杂志 2018年24卷第3期页码：166-172
- 作者机构：
- 作者简介：
- 基金信息：
  
  国家自然科学基金项目（81374064）
- DOI：10.13422/j.cnki.syfjx.2018030166
  中图分类号： R285.5
- 纸质出版日期：2018
- 稿件说明：
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李梅, 陈慧, 柯才华, 等. 金不换与雪上一枝蒿不同比例配伍的减毒增效作用[J]. 中国实验方剂学杂志, 2018,24(3):166-172.

LI Mei, CHEN Hui, KE Cai-hua, et al. Decreasing Toxicity and Increasing Efficacy Through Different Compatibilities of and [J]. Chinese journal of experimental traditional medical formulae, 2018, 24(3): 166-172.
李梅, 陈慧, 柯才华, 等. 金不换与雪上一枝蒿不同比例配伍的减毒增效作用[J]. 中国实验方剂学杂志, 2018,24(3):166-172. DOI： 10.13422/j.cnki.syfjx.2018030166.

LI Mei, CHEN Hui, KE Cai-hua, et al. Decreasing Toxicity and Increasing Efficacy Through Different Compatibilities of and [J]. Chinese journal of experimental traditional medical formulae, 2018, 24(3): 166-172. DOI： 10.13422/j.cnki.syfjx.2018030166.

摘要

目的：探讨金不换水提物（WVBF）配伍雪上一枝蒿总生物碱（CFA）的解毒作用及对药效的影响。方法：建立斑马鱼心血管模型，评价心血管毒性；上下法测小鼠不同比例CFA-WVBF的半数致死量（LD50）；以热板法和扭体法比较CFA-WVBF 1∶2和1∶5配伍组对小鼠中枢和外周镇痛作用的影响。结果：在心血管毒性评价实验中，单药CFA除了200 mg·L-1组外，别的质量浓度组对斑马鱼心率都没有影响，不诱发斑马鱼心律不齐，CFA 66.6，200 mg·L-1可诱发斑马鱼毒性表型（P<0.05）。在不同配伍组心血管毒性评价实验中，除了CFA-WVBF 1∶5配伍组，别的实验组都诱发明显的心血管毒性表型（P<0.05）。CFA-WVBF 4个不同比例（5∶1，2∶1，1∶2，1∶5）的LD50依次增加，都高于单独CFA的LD50（P<0.05）。在中枢镇痛实验中，CFA-WVBF按1∶2和1∶5配伍组均可提高小鼠的舔足痛阈值，其中按CFA-WVBF 1∶2混合给药组（20 mg·kg-1）的镇痛率比单独给予CFA （20 mg·kg-1）和阿司匹林组（200 mg·kg-1）的镇痛率要高（P<0.05），而在给药90 min时1∶2配伍组的镇痛率与CFA组接近，都高于阿司匹林组（P<0.05），说明CFA-WVBF 1∶2配伍组有减毒存效作用，按1∶5给药的镇痛率比单独给CFA明显增高，在30，60，90 min也逐渐增加（P<0.05），说明CFA-WVBF 1∶5配伍组有减毒增效和延效作用。在外周镇痛方面，各配伍给药组均能有效抑制冰乙酸所致小鼠扭体反应，其中CFA-WVBF 1∶2配伍组的扭体抑制率低于单独给予CFA组（P<0.05）；CFA-WVBF 1∶5配伍组的扭体抑制率略高于CFA组（P<0.05）。表明在外周镇痛方面，CFA-WVBF 1∶2配伍组有减毒减效作用，CFA-WVBF 1∶5配伍组有较弱的减毒增效作用。结论：CFA-WVBF配伍可以减轻CFA诱发的斑马鱼心血管毒性和小鼠急性毒性，CFA-WVBF 1∶2，1∶5配伍组可以提高中枢镇痛效应，CFA-WVBF 1∶5配伍组还可以增加外周镇痛作用，因此CFA-WVBF 1∶5配伍组减毒增效作用最好。

Abstract

Objective:To investigate the detoxication effect and efficacy of water extract from Veratrilla baillonii(WVBF) with compatibility of total alkaloids from Aconitum brachypodum(CFA). Method:The cardiovascular toxicity was evaluated by using zebra fish cardiovascular model; up-and-down method was used to calculate the median lethal dose (LD50) of CFA and WVBF of different compatibility proportions; then acetic acid induced writhing response and hot plate method were used to observe and compare the central and peripheral analgesic effects of CFA-WVBF 1:2 group and CFA-WVBF 1:5 group. Result:In cardiovascular toxicity evaluation experiment

if CFA was used alone

it had no effect on heart rate and did not induce arrhythmia of zebra fish except 200 mg·L-1 group; 66.6

200 mg·L-1 groups induced toxicity phenotype (P<0.05). In different compatibilities experiment

all the experimental groups induced obvious cardiovascular toxicity except CFA-WVBF 1:5 group (P<0.05). The LD50 of CFA-WVBF compatibilities (5:1

2:1

1:2

1:5) was increasing in turn

and all of them were higher than the LD50 of CFA alone (P<0.05). In the central analgesia experiment

CFA-WVBF 1:2 group and CFA-WVBF 1:5 group can enhance foot pain threshold

and the analgesia effects of CFA-WVBF 1:2 group (CFA-WVBF

20 mg·kg-1) were better than those of CFA (20 mg·kg-1) alone group and aspirin group (200 mg·kg-1)

but the analgesia percentage in CFA-WVBF 1:2 group was similar to that in CFA group and higher than that in aspirin group (P<0.05) after 90 minutes

indicating that CFA-WVBF 1:2 group could reduce toxicity and keep efficacy. The analgesia percentage in CFA-WVBF 1:5 group was higher than that in the CFA alone (20 mg·kg-1) group

and was gradually increased after 30

90 minutes

indicating that CFA-WVBF 1:5 group could reduce toxicity

enhance efficacy and extend efficacy (P<0.05). In peripheral analgesia experiment

different proportions of CFA and WVBF groups could inhibit acetic acid induced writhing response. The writhing inhibition rate in CFA-WVBF 1:2 group was lower than that of CFA alone group (P<0.05); and the writhing inhibition rate in CFA-WVBF 1:5 group was slightly higher than that of CFA alone group (P<0.05)

indicating that the CFA-WVBF 1:2 group could reduce toxicity and decrease efficacy but the CFA-WVBF 1:5 group could reduce toxicity and enhance analgesic efficacy slightly (P<0.05). Conclusion:Different compatibilities of CFA and WVBF can decrease CFA-induced cardiovascular toxicity in zebra fish and acute toxicity in mice; CFA-WVBF 1:2 group and CFA-WVBF 1:5 group can increase central analgesic efficacy

and CFA-WVBF 1:5 group also can enhance peripheral analgesic efficacy. Therefore

CFA-WVBF 1:5 group shows the best effect in decreasing toxicity and increasing efficacy.

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