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维拉帕米对阿霉素诱导的小鼠心脏死亡率及电解质变化的影响。

Effects of verapamil on doxorubicin-induced mortality and electrolyte changes in the mouse heart.

作者信息

Giri S N, Marafino B J

出版信息

Drug Chem Toxicol. 1984;7(4):407-22. doi: 10.3109/01480548408998267.

Abstract

The effects of verapamil on doxorubicin-induced mortality and electrolyte changes were investigated in mice using either 0, 8, 16, or 32 mg/kg verapamil. The verapamil doses were injected by subcutaneous route 24 and 3 hr prior to administration of a single dose of doxorubicin (20 mg/kg, IP), followed by daily treatment with verapamil for 20 subsequent days. Using total deaths or changes in ventricular electrolyte levels as indices of toxicity, there was no evidence that verapamil decreased doxorubicin toxicity. At this dose, doxorubicin increased myocardial calcium and sodium, and decreased magnesium and potassium. Verapamil alone was shown to significantly reduce total ventricular calcium and increase magnesium in a dose-dependent manner. The ventricular sodium and potassium levels were not affected by verapamil treatment. Neither the increase in calcium nor the decrease in heart magnesium content of the ventricles in response to doxorubicin, was lessened by verapamil treatment. Doxorubicin-associated sodium increase in ventricular tissue was greater in groups receiving higher doses of verapamil but decrease of potassium in the ventricles of these animals remained unaffected. We conclude from the findings of the present study that verapamil is inappropriate as an antagonist of the cardiac toxicity resulting from treatment with doxorubicin.

摘要

使用0、8、16或32毫克/千克维拉帕米,在小鼠中研究了维拉帕米对阿霉素诱导的死亡率和电解质变化的影响。维拉帕米剂量在单次给予阿霉素(20毫克/千克,腹腔注射)前24小时和3小时通过皮下途径注射,随后连续20天每天用维拉帕米治疗。以总死亡数或心室电解质水平变化作为毒性指标,没有证据表明维拉帕米降低了阿霉素毒性。在此剂量下,阿霉素增加心肌钙和钠含量,并降低镁和钾含量。单独使用维拉帕米显示可显著降低心室总钙含量,并以剂量依赖方式增加镁含量。维拉帕米治疗未影响心室钠和钾水平。维拉帕米治疗既未减轻阿霉素引起的钙增加,也未减轻心室心脏镁含量的降低。在接受较高剂量维拉帕米的组中,阿霉素相关的心室组织钠增加更大,但这些动物心室中的钾降低仍未受影响。根据本研究结果,我们得出结论,维拉帕米不适合作为阿霉素治疗所致心脏毒性的拮抗剂。

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