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药物特异性F(ab')2片段可降低大鼠体内地昔帕明的心脏毒性。

Drug-specific F(ab')2 fragment reduces desipramine cardiotoxicity in rats.

作者信息

Brunn G J, Keyler D E, Ross C A, Pond S M, Pentel P R

机构信息

Minneapolis Medical Research Foundation, Minnesota.

出版信息

Int J Immunopharmacol. 1991;13(7):841-51. doi: 10.1016/0192-0561(91)90035-6.

Abstract

Current therapy for cardiotoxicity due to tricyclic antidepressant (TCA) overdose is often ineffective in seriously poisoned patients. We studied the effect of a drug-specific antibody fragment on TCA cardiotoxicity in rats. Animals received anti-TCA F(ab')2 2.0 g/kg i.v. over 10 min starting 15 min after administration of a toxic dose of desipramine (DMI). This anti-TCA F(ab')2 dose was 36.9% of the molar DMI dose in terms of binding sites. Anti-TCA F(ab')2 infusion had no adverse effects and rapidly reduced DMI induced QRS prolongation compared with control F(ab')2 (23 +/- 14 vs 71 +/- 11% QRS prolongation at the end of infusion, P less than 0.001). This beneficial effect lasted for the 45 min duration of the study. Markedly enhanced DMI binding in serum after anti-TCA F(ab')2 was demonstrated by a 48-fold increase in the total DMI concentration over controls and a reduction in the fraction of unbound DMI (44.5 +/- 19.4 vs 0.7 +/- 0.2%). Anti-TCA F(ab')2 reduced the DMI concentration in brain but not in other organs. We conclude that anti-TCA F(ab')2 substantially reduces DMI cardiotoxicity in rats, and does so rapidly enough to be of potential clinical benefit for patients with DMI overdose. Because only a small fraction of the DMI dose was bound by antibody, these data suggest that antibody fragment doses considerably less than equimolar to the DMI dose may be effective in treating DMI cardiotoxicity.

摘要

三环类抗抑郁药(TCA)过量所致心脏毒性的当前治疗方法,对重度中毒患者往往无效。我们研究了一种药物特异性抗体片段对大鼠TCA心脏毒性的影响。动物在给予致死剂量的地昔帕明(DMI)15分钟后,于10分钟内静脉注射2.0 g/kg抗TCA F(ab')2。就结合位点而言,该抗TCA F(ab')2剂量为DMI摩尔剂量的36.9%。与对照F(ab')2相比,抗TCA F(ab')2输注无不良反应,且能迅速减轻DMI诱导的QRS波增宽(输注结束时QRS波增宽分别为23±14%和71±11%,P<0.001)。这种有益效果在研究的45分钟内持续存在。抗TCA F(ab')2后血清中DMI结合显著增强,表现为总DMI浓度比对照增加48倍,未结合DMI的比例降低(分别为44.5±19.4%和0.7±0.2%)。抗TCA F(ab')2降低了脑内DMI浓度,但其他器官中的浓度未降低。我们得出结论,抗TCA F(ab')2可显著降低大鼠DMI心脏毒性,且起效足够快,对DMI过量患者可能具有潜在临床益处。由于只有一小部分DMI剂量被抗体结合,这些数据表明,抗体片段剂量远低于DMI剂量的等摩尔量,可能对治疗DMI心脏毒性有效。

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