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Prevention of the pulmonary vasoconstrictor effects of HBOC-201 in awake lambs by continuously breathing nitric oxide.

机译:通过持续呼吸一氧化氮来预防清醒羔羊中HBOC-201的肺血管收缩作用。

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BACKGROUND: Hemoglobin-based oxygen-carrying solutions (HBOC) provide emergency alternatives to blood transfusion to carry oxygen to tissues without the risks of disease transmission or transfusion reaction. Two primary concerns hampering the clinical acceptance of acellular HBOC are the occurrence of systemic and pulmonary vasoconstriction and the maintenance of the heme-iron in the reduced state (Fe2+). We recently demonstrated that pretreatment with inhaled nitric oxide prevents the systemic hypertension induced by HBOC-201 (polymerized bovine hemoglobin) infusion in awake mice and sheep without causing methemoglobinemia. However, the impact of HBOC-201 infusion with or without inhaled nitric oxide on pulmonary vascular tone has not yet been examined. METHODS: The pulmonary and systemic hemodynamic effects of breathing nitric oxide both before and after the administration of HBOC-201 were determined in healthy, awake lambs. RESULTS: Intravenous administration of HBOC-201 (12 ml/kg) induced prolongedsystemic and pulmonary vasoconstriction. Pretreatment with inhaled nitric oxide (80 parts per million [ppm] for 1 h) prevented the HBOC-201--induced increase in mean arterial pressure but not the increase of pulmonary arterial pressure, systemic vascular resistance, or pulmonary vascular resistance. Pretreatment with inhaled nitric oxide (80 ppm for 1 h) followed by breathing a lower concentration of nitric oxide (5 ppm) during and after HBOC-201 infusion prevented systemic and pulmonary vasoconstriction without increasing methemoglobin levels. CONCLUSIONS: These findings demonstrate that pretreatment with inhaled nitric oxide followed by breathing a lower concentration of the gas during and after administration of HBOC-201 may enable administration of an acellular hemoglobin substitute without vasoconstriction while preserving its oxygen-carrying capacity.
机译:背景:基于血红蛋白的载氧溶液(HBOC)提供了输血的紧急替代方案,可将氧气携带到组织中,而无疾病传播或输血反应的风险。阻碍脱细胞HBOC临床接受的两个主要问题是全身性和肺血管收缩的发生以及血红素铁在还原状态(Fe2 +)的维持。我们最近证明,采用吸入一氧化氮进行的预处理可防止在清醒的小鼠和绵羊中注射HBOC-201(聚合牛血红蛋白)引起的系统性高血压,而不会引起高铁血红蛋白血症。然而,尚未检查过是否有吸入一氧化氮的HBOC-201输注对肺血管张力的影响。方法:测定健康清醒的羔羊在服用HBOC-201之前和之后呼吸一氧化氮对肺和全身的血流动力学影响。结果:静脉注射HBOC-201(12 ml / kg)可导致全身和肺血管收缩时间延长。吸入一氧化氮(百万分之80 [ppm] 1 h)进行的预处理可防止HBOC-201引起的平均动脉压升高,但不能阻止肺动脉压,全身血管阻力或肺血管阻力的增加。在HBOC-201输注期间和之后,使用吸入一氧化氮(80 ppm进行1小时)预处理,然后呼吸较低浓度的一氧化氮(5 ppm),可以防止全身和肺血管收缩,而不会增加高铁血红蛋白水平。结论:这些发现表明,在服用HBOC-201期间和之后,用吸入一氧化氮进行预处理,然后呼吸较低浓度的气体,可以在无血管收缩的情况下使用无细胞血红蛋白替代品,同时保持其携氧能力。

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