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Hemoglobin-based oxygen carriers: from mechanisms of toxicity and clearance to rational drug design.

机译:基于血红蛋白的氧气载体:从毒性和清除机制到合理的药物设计。

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摘要

Hemoglobin-based oxygen carriers (HBOCs) have been developed to support blood oxygen transport capacity during hemorrhagic shock, hemolysis and ischemic insult. Existing product candidates have demonstrated considerable efficacy in experimental animal models and in clinical trial subjects; however, severe adverse safety signals that appeared in recent phase II and phase III clinical trials involving certain HBOCs have in part hindered further development and licensing. Emerging insights into hemoglobin (Hb) toxicity as well as physiologic Hb scavengers such as haptoglobin and CD163 that are capable of detoxifying extracellular Hb in vivo suggest that alternative product candidates could be designed. Together with novel animal models and biomarkers tailored to monitor the effects of extracellular Hb, a new generation of HBOCs can be envisioned.
机译:已经开发出基于血红蛋白的氧气载体(HBOC),以在失血性休克,溶血和缺血性损伤期间支持血氧转运能力。现有的候选产品在实验动物模型和临床试验受试者中已显示出相当大的功效;但是,最近在涉及某些HBOC的II期和III期临床试验中出现的严重不良安全信号在一定程度上阻碍了进一步的开发和许可。对血红蛋白(Hb)毒性以及能够在体内解毒细胞外Hb的生理性Hb清除剂(如触珠蛋白和CD163)的新见解表明,可以设计替代产品。结合专为监测细胞外Hb的作用而设计的新型动物模型和生物标记,可以设想出新一代的HBOC。

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