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通过持续灌注白细胞介素-1受体拮抗剂提高实验性大鼠中暑后的生存率。

Increased survival in experimental rat heatstroke by continuous perfusion of interleukin-1 receptor antagonist.

作者信息

Chiu W T, Kao T Y, Lin M T

机构信息

Department of Public Health, Taipei Medical College, Taiwan.

出版信息

Neurosci Res. 1996 Jan;24(2):159-63. doi: 10.1016/0168-0102(95)00987-6.

DOI:10.1016/0168-0102(95)00987-6
PMID:8929922
Abstract

In order to assess the possible therapeutical value of interleukin-1 receptor antagonist (IL-1 ra) in the treatment of heatstroke, we evaluated the effects of heatstroke on survival time (interval between onset of heatstroke and death), systemic and striatal hemodynamic changes, and extent of striatal neuronal damage in rats treated with saline or IL-1 ra. The survival time of the heatstroke rats which received normal saline (single injection or continuous perfusion) was about 17 min. The heatstroke-induced ischemic damage to striatal neurons was due to systemic arterial hypotension, intracranial hypertension, decreased cerebral perfusion, and striatal dopamine (DA) accumulation (275%). Rats treated with a single injection of IL-1 ra (200 mu g/kg, i.v.) immediately after the onset of heatstroke survived much longer (91 min) than the controls. The prolongation of survival induced by IL-1 ra was brought about by attenuation of the arterial hypotension, intracranial hypertension, decreased cerebral perfusion, ischemic damage to striatal neurons, and striatal DA release value (204%). Furthermore, after continuous perfusion of IL-1 ra (200 mu g/kg per h, i.v.) immediately after the onset of heatstroke, the striatal DA release value of the rats was further reduced to 140% while the survival time of the rats was prolonged to up to 10 h from the onset of heatstroke. Thus, it appears that continuous i.v. perfusion of IL-1 ra is a good choice for heatstroke therapy.

摘要

为了评估白细胞介素-1受体拮抗剂(IL-1ra)在治疗中暑方面的潜在治疗价值,我们评估了中暑对用生理盐水或IL-1ra处理的大鼠存活时间(中暑发作至死亡的间隔时间)、全身和纹状体血流动力学变化以及纹状体神经元损伤程度的影响。接受生理盐水(单次注射或持续灌注)的中暑大鼠的存活时间约为17分钟。中暑诱导的纹状体神经元缺血性损伤是由于全身动脉低血压、颅内高压、脑灌注减少以及纹状体多巴胺(DA)积累(275%)。中暑发作后立即单次注射IL-1ra(200μg/kg,静脉注射)的大鼠比对照组存活时间长得多(91分钟)。IL-1ra诱导的存活时间延长是由于动脉低血压、颅内高压、脑灌注减少、纹状体神经元缺血性损伤以及纹状体DA释放值(204%)的减轻。此外,中暑发作后立即持续灌注IL-1ra(200μg/kg每小时,静脉注射),大鼠的纹状体DA释放值进一步降至140%,而大鼠的存活时间从中暑发作起延长至长达10小时。因此,静脉持续灌注IL-1ra似乎是中暑治疗的一个不错选择。

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