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Polynitroxylated pegylated hemoglobin: a novel neuroprotective hemoglobin for acute volume-limited fluid resuscitation after combined traumatic brain injury and hemorrhagic hypotension in mice.

机译:多硝基氧化聚乙二醇化血红蛋白:一种新型的神经保护性血红蛋白,可用于小鼠颅脑外伤和出血性低血压合并后的急性容量受限的液体复苏。

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OBJECTIVE: Resuscitation of hemorrhagic hypotension after traumatic brain injury is challenging. A hemoglobin-based oxygen carrier may offer advantages. The novel therapeutic hemoglobin-based oxygen carrier, polynitroxylated pegylated hemoglobin (PNPH), may represent a neuroprotective hemoglobin-based oxygen carrier for traumatic brain injury resuscitation. HYPOTHESES: 1) PNPH is a unique non-neurotoxic hemoglobin-based oxygen carrier in neuronal culture and is neuroprotective in in vitro neuronal injury models. 2) Resuscitation with PNPH would require less volume to restore mean arterial blood pressure than lactated Ringer's or Hextend and confer neuroprotection in a mouse model of traumatic brain injury plus hemorrhagic hypotension. DESIGN: Prospective randomized, controlled experimental study. SETTING: University center. MEASUREMENTS AND MAIN RESULTS: In rat primary cortical neuron cultures, control bovine hemoglobin was neurotoxic (lactate dehydrogenase release; 3-[4,5-dimethylthiazol-2-yl-]-2,5-diphenyltetrazolium bromide assay) at concentrations from 12.5 to 0.625 muM, whereas polyethylene glycol-conjugated hemoglobin showed intermediate toxicity. PNPH was not neurotoxic (p<.05 vs. bovine hemoglobin and polyethylene glycol hemoglobin; all concentrations). PNPH conferred neuroprotection in in vitro neuronal injury (glutamate/glycine exposure and neuronal stretch), as assessed via lactate dehydrogenase and 3-[4,5-dimethylthiazol-2-yl-]-2,5-diphenyltetrazolium bromide (all p<.05 vs. control). C57BL6 mice received controlled cortical impact followed by hemorrhagic hypotension (2 mL/100 g, mean arterial blood pressure approximately 35-40 mm Hg) for 90 min. Mice were resuscitated (mean arterial blood pressure>50 mm Hg for 30 min) with lactated Ringer's, Hextend, or PNPH, and then shed blood was reinfused. Mean arterial blood pressures, resuscitation volumes, blood gasses, glucose, and lactate were recorded. Brain sections at 7 days were examined via hematoxylin and eosin and Fluoro-Jade C (identifying dying neurons) staining in CA1 and CA3 hippocampus. Resuscitation with PNPH or Hextend required less volume than lactated Ringer's (both p<.05). PNPH but not Hextend improved mean arterial blood pressure vs. lactated Ringer's (p<.05). Mice resuscitated with PNPH had fewer Fluoro-Jade C positive neurons in CA1 vs. Hextend and lactated Ringer's, and CA3 vs. Hextend (p<.05). CONCLUSIONS: PNPH is a novel neuroprotective hemoglobin-based oxygen carrier in vitro and in vivo that may offer unique advantages for traumatic brain injury resuscitation.
机译:目的:颅脑外伤后出血性低血压的复苏具有挑战性。基于血红蛋白的氧气载体可能具有优势。新型的基于治疗性血红蛋白的氧气载体,多硝基氧化聚乙二醇化血红蛋白(PNPH),可能代表一种用于创伤性脑损伤复苏的神经保护性基于血红蛋白的氧气载体。假设:1)PNPH是神经元培养物中独特的基于非神经毒性血红蛋白的氧载体,在体外神经元损伤模型中具有神经保护作用。 2)在患有外伤性脑损伤加出血性低血压的小鼠模型中,用PNPH复苏比恢复乳酸林格氏或Hextend所需的体积更小,以恢复平均动脉血压,并赋予神经保护作用。设计:前瞻性随机对照实验研究。地点:大学中心。测量和主要结果:在大鼠原代皮层神经元培养物中,对照牛血红蛋白对神经毒性(乳酸脱氢酶释放; 3- [4,5-二甲基噻唑-2-基-]-2,5-二苯基四唑溴化物测定)的浓度为12.5至0.625μM,而聚乙二醇缀合的血红蛋白显示中等毒性。 PNPH无神经毒性(相对于牛血红蛋白和聚乙二醇血红蛋白,p <0.05);所有浓度。通过乳酸脱氢酶和3- [4,5-二甲基噻唑-2-基-]-2,5-二苯基四唑溴化物评估,PNPH在体外神经元损伤(谷氨酸/甘氨酸暴露和神经元伸展)中赋予了神经保护作用(所有p <。 05与对照)。 C57BL6小鼠受到可控的皮质撞击,随后出现出血性低血压(2 mL / 100 g,平均动脉血压约为35-40 mm Hg),持续90分钟。用乳酸林格氏,Hextend或PNPH对小鼠进行复苏(平均动脉血压> 50 mm Hg,持续30分钟),然后重新注入流血的血液。记录平均动脉血压,复苏量,血气,葡萄糖和乳酸。通过苏木精和曙红和CA1和CA3海马中的Fluoro-Jade C(识别垂死的神经元)染色检查了第7天的大脑切片。用PNPH或Hextend进行复苏所需的体积要小于乳酸林格氏液(均p <.05)。与乳酸林格氏症相比,PNPH改善了平均动脉血压,但Hextend并未改善(p <.05)。用PNPH复苏的小鼠在CA1相对于Hextend和乳酸林格氏液中的Fluoro-Jade C阳性神经元较少,在CA3相对于Hextend时则较少(p <.05)。结论:PNPH是一种新型的基于神经保护性血红蛋白的氧载体,在体外和体内均可为创伤性脑损伤复苏提供独特的优势。

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