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二聚体交联人血红蛋白的毒副作用可被去辅基血红蛋白-触珠蛋白复合物减弱。

Toxic side-effects of diaspirin cross-linked human hemoglobin are attenuated by the apohemoglobin-haptoglobin complex.

机构信息

Department of Bioengineering, University of California San Diego, La Jolla, CA, United States.

William G. Lowrie Department of Chemical and Biomolecular Engineering, The Ohio State University, Columbus, OH, United States.

出版信息

Biomed Pharmacother. 2024 May;174:116569. doi: 10.1016/j.biopha.2024.116569. Epub 2024 Apr 10.

DOI:10.1016/j.biopha.2024.116569
PMID:38603886
Abstract

Alpha-alpha diaspirin-crosslinked human hemoglobin (DCLHb or ααHb) was a promising early generation red blood cell (RBC) substitute. The DCLHb was developed through a collaborative effort between the United States Army and Baxter Healthcare. The core design feature underlying its development was chemical stabilization of the tetrameric structure of hemoglobin (Hb) to prevent Hb intravascular dimerization and extravasation. DCLHb was developed to resuscitate warfighters on the battlefield, who suffered from life-threatening blood loss. However, extensive research revealed toxic side effects associated with the use of DCLHb that contributed to high mortality rates in clinical trials. This study explores whether scavenging Hb and heme via the apohemoglobin-haptoglobin (apoHb-Hp) complex can reduce DCLHb associated toxicity. Awake Golden Syrian hamsters were equipped with a window chamber model to characterize the microcirculation. Each group was first infused with either Lactated Ringer's or apoHb-Hp followed by a hypovolemic infusion of 10% of the animal's blood volume of DCLHb. Our results indicated that animals pretreated with apoHb-Hb exhibited improved microhemodynamics vs the group pretreated with Lactated Ringer's. While systemic acute inflammation was observed regardless of the treatment group, apoHb-Hp pretreatment lessened those effects with a marked reduction in IL-6 levels in the heart and kidneys compared to the control group. Taken together, this study demonstrated that utilizing a Hb and heme scavenger protein complex significantly reduces the microvasculature effects of ααHb, paving the way for improved HBOC formulations. Future apoHb-Hp dose optimization studies may identify a dose that can completely neutralize DCLHb toxicity.

摘要

αα-二联阿司匹林交联人血红蛋白(DCLHb 或 ααHb)是一种很有前途的第一代红细胞(RBC)替代品。DCLHb 是由美国陆军和百特医疗保健公司合作开发的。其开发的核心设计特点是化学稳定血红蛋白(Hb)的四聚体结构,以防止 Hb 血管内二聚化和外渗。DCLHb 的开发是为了在战场上抢救遭受危及生命的失血的战斗人员。然而,广泛的研究揭示了与使用 DCLHb 相关的毒性副作用,这导致临床试验中的高死亡率。本研究探讨了通过去氧血红蛋白-触珠蛋白(apoHb-Hp)复合物清除 Hb 和血红素是否可以降低 DCLHb 相关毒性。给清醒的金黄叙利亚仓鼠配备了一个窗室模型来描述微循环。每组首先输注乳酸林格氏液或 apoHb-Hp,然后进行 10%动物血容量的 DCLHb 低血容量输注。我们的结果表明,用 apoHb-Hp 预处理的动物表现出改善的微循环动力学,与用乳酸林格氏液预处理的组相比。尽管无论治疗组如何,都观察到全身性急性炎症,但 apoHb-Hp 预处理减轻了这些影响,与对照组相比,心脏和肾脏中的 IL-6 水平明显降低。总之,这项研究表明,利用 Hb 和血红素清除蛋白复合物可显著减轻 ααHb 对微血管的影响,为改进 HBOC 配方铺平道路。未来的 apoHb-Hp 剂量优化研究可能会确定一个可以完全中和 DCLHb 毒性的剂量。

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