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Hemoglobin-Based Blood Substitutes and the Treatment of Sickle Cell Disease: More Harm than Help?

机译:基于血红蛋白的血液替代品和镰状细胞病的治疗:危害大于帮助?

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摘要

Intense efforts have been made by both industry and academia over the last three decades to produce viable hemoglobin (Hb)-based oxygen carriers (HBOCs), also known as “blood substitutes”. Human trials conducted so far by several manufactures in a variety of clinical indications, including trauma, and elective surgeries have failed and no product has gained the Food and Drug Administration approval for human use. Safety concerns due to frequent incidences of hemodynamic, cardiac events, and even death led to the termination of some of these trials. Several second generation HBOC products that have been chemically and/or genetically modified (or in some cases ligated with carbon monoxide (CO)) found a new clinical application in conditions as complex as sickle cell disease (SCD). By virtue of higher oxygen affinity (P50) (R-state), and smaller size, HBOCs may be able to reach the microvasculature unload of oxygen to reverse the cycles of sickling/unsickling of the deoxy-sickle cell Hb (HbS) (T-state), thus preventing vaso-occlusion, a central event in SCD pathophysiology. However, biochemically, it is thought that outside the red blood cell (due to frequent hemolysis), free HbS or infused HBOCs are capable of interfering with a number of oxidative and signaling pathways and may, thus, negate any benefit that HBOCs may provide. This review discusses the advantages and disadvantages of using HBOCs in SCD.
机译:在过去的三十年中,工业界和学术界都做出了巨大的努力,以生产基于活血红蛋白(Hb)的氧气载体(HBOC),也被称为“血液替代品”。迄今为止,多家制造商在包括外伤在内的各种临床适应症中进行的人体试验和选择性外科手术均告失败,没有产品获得美国食品药品监督管理局的批准。由于血液动力学,心脏事件甚至死亡的频繁发生而引起的安全隐患导致其中一些试验终止。经过化学和/或基因修饰(或在某些情况下与一氧化碳(CO)连接)的几种第二代HBOC产品在镰状细胞病(SCD)等复杂条件下获得了新的临床应用。由于较高的氧亲和力(P50)(R状态)和较小的尺寸,HBOC可能能够达到氧的微脉管系统卸载,从而逆转脱氧镰刀细胞Hb(HbS)(T -状态),从而防止血管闭塞,这是SCD病理生理学的中心事件。但是,从生化角度看,据认为在红细胞外部(由于频繁的溶血),游离的HbS或注入的HBOC能够干扰许多氧化和信号传导途径,因此可能会抵消HBOC可能提供的任何益处。这篇评论讨论了在SCD中使用HBOC的优缺点。

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