Systemic administration of recombinant erythropoietin (EPO) has bee'/> A single subcutaneous bolus of erythropoietin normalizes cerebral blood flow autoregulation after subarachnoid haemorrhage in rats
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A single subcutaneous bolus of erythropoietin normalizes cerebral blood flow autoregulation after subarachnoid haemorrhage in rats

机译:蛛网膜下腔出血后单次皮下注射促红细胞生成素可使脑血流自动调节正常

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摘要

class="enumerated" style="list-style-type:decimal">Systemic administration of recombinant erythropoietin (EPO) has been demonstrated to mediate neuroprotection. This effect of EPO may in part rely on a beneficial effect on cerebrovascular dysfunction leading to ischaemic neuronal damage. We investigated the in vivo effects of subcutaneously administered recombinant EPO on impaired cerebral blood flow (CBF) autoregulation after experimental subarachnoid haemorrhage (SAH).Four groups of male Sprague-Dawley rats were studied: group A, sham operation plus vehicle; group B, sham operation plus EPO; group C, SAH plus vehicle; group D, SAH plus EPO. SAH was induced by injection of 0.07 ml of autologous blood into the cisterna magna. EPO (400 iu kg−1 s.c.) or vehicle was given immediately after the subarachnoid injection of blood or saline. Forty-eight hours after the induction of SAH, CBF autoregulatory function was evaluated using the intracarotid 133Xe method.CBF autoregulation was preserved in both sham-operated groups (lower limits of mean arterial blood pressure: 91±3 and 98±3 mmHg in groups A and B, respectively). In the vehicle treated SAH-group, autoregulation was abolished and the relationship between CBF and blood pressure was best described by a single linear regression line. A subcutaneous injection of EPO given immediately after the induction of SAH normalized autoregulation of CBF (lower limit in group D: 93±4 mmHg, NS compared with groups A and B).Early activation of endothelial EPO receptors may represent a potential therapeutic strategy in the treatment of cerebrovascular perturbations after SAH.
机译:class =“ enumerated” style =“ list-style-type:decimal”> <!-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 重组促红细胞生成素(EPO)的全身给药已被证明可以介导神经保护作用。 EPO的这种作用可能部分取决于对导致缺血性神经元损害的脑血管功能障碍的有益作用。我们研究了皮下注射重组EPO对实验性蛛网膜下腔出血(SAH)后脑血流量(CBF)自动调节受损的体内作用。 研究了四组雄性Sprague-Dawley大鼠:A组,假手术操作加车辆; B组,假手术加EPO; C组,SAH加车辆; D组,SAH加EPO。 SAH是通过向大水罐中注入0.07微克自体血来诱导的。蛛网膜下腔注射血液或盐水后立即给予EPO(400 iu kg -1 s.c.)。 SAH诱导后48小时,采用颈内 133 Xe方法评估CBF的自动调节功能。 两个假手术组均保留了CBF的自动调节功能(下限为平均动脉血压:A组和B组分别为91±3和98±3 mmHg。在用媒介物治疗的SAH组中,取消了自动调节功能,而CBF与血压之间的关系最好用一条线性回归线来描述。 SAH诱导后立即皮下注射EPO,使CBF的自律调节正常(D组下限:93±4 mmHg,NS与A和B组相比)。 内皮EPO受体的早期活化可能代表SAH后脑血管微扰的潜在治疗策略。

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