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在麻醉的棕色挪威大鼠过敏性休克模型中,比较精氨酸加压素、特利加压素或肾上腺素纠正低血压的效果。

Comparison of arginine vasopressin, terlipressin, or epinephrine to correct hypotension in a model of anaphylactic shock in anesthetized brown Norway rats.

作者信息

Dewachter Pascale, Jouan-Hureaux Valérie, Lartaud Isabelle, Bello Gaëlle, de Talancé Nicole, Longrois Dan, Mertes Paul Michel

机构信息

Pôle d'Anesthésie-Réanimation, Centre Hospitalier Universitaire (CHU), Nancy, France.

出版信息

Anesthesiology. 2006 Apr;104(4):734-41. doi: 10.1097/00000542-200604000-00018.

Abstract

BACKGROUND

Arginine vasopressin (AVP) and terlipressin were proposed as alternatives to catecholamines in shock states characterized by decreased plasma AVP concentrations. The endogenous plasma AVP profile in anaphylactic shock is unknown. In an ovalbumin-sensitized anesthetized anaphylactic shock rat model, the authors investigated (1) plasma AVP concentrations and (2) the dose versus mean arterial pressure response for exogenous AVP and terlipressin and compared them with those of epinephrine.

METHODS

In a first series of rats (n = 12), endogenous plasma AVP concentrations were compared with a model of pharmacologically induced hypotension (nicardipine, n = 12). A second series was randomly assigned to three groups (AVP, n = 7; terlipressin, n = 7; epinephrine, n = 7) and dose (AVP: 8 doses, 0.03-100 U/kg; terlipressin: 7 doses, 0.03-30 microg/kg; epinephrine: 7 doses, 0.3-300 microg/kg)-response mean arterial pressure curves were plotted. Data are expressed as mean +/- SD.

RESULTS

Endogenous plasma AVP concentrations were significantly lower in anaphylactic shock (57 +/- 26 pg/ml) than in the nicardipine group (91 +/- 43 pg/ml; P < 0.05). The ED50 was 10.6 microg/kg (95% confidence interval, 7.1-15.9) for epinephrine and 4.1 U/kg (95% confidence interval, 3.0-5.6) for AVP. Terlipressin did not change mean arterial pressure, regardless of the dose used.

CONCLUSIONS

In a rat model, anaphylactic shock is associated with inadequately low plasma AVP concentrations. For clinically relevant doses, AVP and epinephrine had comparable effects on mean arterial pressure and heart rate values, whereas, unexpectedly, terlipressin was ineffective. These results are consistent with reports in humans experiencing anaphylaxis where AVP injection restored arterial pressure.

摘要

背景

在以血浆精氨酸加压素(AVP)浓度降低为特征的休克状态下,精氨酸加压素和特利加压素被提议作为儿茶酚胺的替代药物。过敏性休克时内源性血浆AVP情况尚不清楚。在卵清蛋白致敏的麻醉过敏性休克大鼠模型中,作者研究了:(1)血浆AVP浓度;(2)外源性AVP和特利加压素的剂量与平均动脉压反应,并将它们与肾上腺素的情况进行比较。

方法

在第一组大鼠(n = 12)中,将内源性血浆AVP浓度与药理学诱导的低血压模型(尼卡地平,n = 12)进行比较。第二组随机分为三组(AVP组,n = 7;特利加压素组,n = 7;肾上腺素组,n = 7),绘制剂量(AVP:8个剂量,0.03 - 100 U/kg;特利加压素:7个剂量,0.03 - 30 μg/kg;肾上腺素:7个剂量,0.3 - 300 μg/kg)-反应平均动脉压曲线。数据以均值±标准差表示。

结果

过敏性休克时内源性血浆AVP浓度(57±26 pg/ml)显著低于尼卡地平组(91±43 pg/ml;P < 0.05)。肾上腺素的半数有效剂量(ED50)为10.6 μg/kg(95%置信区间,7.1 - 15.9),AVP为4.1 U/kg(95%置信区间,3.0 - 5.6)。无论使用何种剂量,特利加压素均未改变平均动脉压。

结论

在大鼠模型中,过敏性休克与血浆AVP浓度过低有关。对于临床相关剂量,AVP和肾上腺素对平均动脉压和心率值具有相似的作用,而意外的是,特利加压素无效。这些结果与人类过敏性反应的报道一致,即注射AVP可恢复动脉压。

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