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创伤性休克中的阿片类拮抗剂。

Opiate antagonist in traumatic shock.

作者信息

McIntosh T K, Faden A I

出版信息

Ann Emerg Med. 1986 Dec;15(12):1462-5. doi: 10.1016/s0196-0644(86)80944-1.

Abstract

In experimental animal studies, opiate receptor antagonists (such as naloxone) and physiological opiate antagonists (thyrotropin-releasing hormone [TRH] have been used with some success to improve outcome and physiological variables following traumatic shock associated with hypovolemia, spinal cord trauma, and head injury. Naloxone at high doses (in the mg/kg range) improves blood pressure and survival following hypovolemic shock in some species subjected to fixed-pressure shock. Similarly, naloxone treatment in the same dose range improves blood pressure and outcome following traumatic spinal shock as well as shock associated with traumatic head injury in selected animal models. The high doses of naloxone required in these studies suggest that the beneficial effects may be due to actions at relatively naloxone-insensitive opiate receptors, such as the kappa-receptor. Changes in the putative kappa-receptor ligand dynorphin are found after hypovolemic shock and traumatic injury to the brain or spinal cord. Opiate receptor antagonists with increased selectivity for the kappa-receptor may be superior to naloxone in the treatment of these conditions. TRH or TRH analogs similarly improve blood pressure and outcome following hypovolemic or spinal shock. Clinical trials of naloxone (at high doses) in human spinal cord injury have begun, and there are plans for clinical trials of naloxone in human head trauma and of TRH in human spinal cord injury.

摘要

在实验动物研究中,阿片受体拮抗剂(如纳洛酮)和生理性阿片拮抗剂(促甲状腺激素释放激素[TRH])已被用于改善与低血容量、脊髓损伤和头部损伤相关的创伤性休克后的预后和生理变量,且取得了一定成功。高剂量(毫克/千克范围)的纳洛酮可改善某些遭受固定压力休克的物种在低血容量休克后的血压和存活率。同样,在选定的动物模型中,相同剂量范围的纳洛酮治疗可改善创伤性脊髓休克以及与创伤性头部损伤相关的休克后的血压和预后。这些研究中所需的高剂量纳洛酮表明,其有益作用可能归因于对相对不敏感的阿片受体(如κ受体)的作用。在低血容量休克以及脑或脊髓创伤性损伤后,可发现假定的κ受体配体强啡肽的变化。对κ受体具有更高选择性的阿片受体拮抗剂在治疗这些病症方面可能优于纳洛酮。TRH或TRH类似物同样可改善低血容量或脊髓休克后的血压和预后。纳洛酮(高剂量)治疗人类脊髓损伤的临床试验已经开始,并且有计划开展纳洛酮治疗人类头部创伤以及TRH治疗人类脊髓损伤的临床试验。

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