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[改良血红蛋白溶液作为人工氧载体]

[Modified hemoglobin solutions as artificial oxygen carriers].

作者信息

Lenz G, Bissinger U

机构信息

Abteilung Anaesthesiologie, Universität Tübingen.

出版信息

Infusionsther Transfusionsmed. 1994 Nov;21 Suppl 3:63-7.

PMID:7841783
Abstract

At least theoretically, hemoglobin (Hb) solutions are ideal colloidal plasma substitutes because of their unique ability to take up oxygen, transport it in bound form, and release it peripherally. The present study gives an overview of the development and present status of modified Hb preparations. While human and bovine erythrocytes are used for production on the one hand, human Hb variants can also be derived from yeast or bacteria as well as via transgenic animals through recombinant DNA technology. The pronounced limitations of extraerythrocytic Hb, that is its high oxygen affinity and its inadequate intravascular persistence, can be overcome by various modifications. Intravascular half-life of free Hb can be significantly increased by intramolecular stabilization, linking to macromolecules, intermolecular cross-linking (PolyHb solutions) or microencapsulation. Oxygen affinity of human Hb may be lowered by coupling of allosteric modulators to the 2,3-bisphosphoglycerate site, e.g. pyridoxal phosphate, whereas bovine Hb has an intrinsically low oxygen affinity. Human pyridoxylated PolyHb solutions and bovine PolyHb solutions presently fulfill at least 2 of the 3 principal requirements for an oxygen-transporting plasma substitute, i.e. maintenance of the circulating blood volume with provision of additionally utilizable oxygen capacity. Matters of concern with all Hb preparations remain potential vasoconstrictive effects and renal toxicity. Major efforts being undertaken at present by industry and research groups give reason to hope, however, that the concept of modified Hb solutions as oxygen carriers will be realized in the foreseeable future.

摘要

至少从理论上讲,血红蛋白(Hb)溶液是理想的胶体血浆代用品,因为它们具有独特的能力,能够摄取氧气,以结合形式运输氧气,并在周边释放氧气。本研究概述了改良血红蛋白制剂的发展情况和现状。一方面,人红细胞和牛红细胞用于生产,而人血红蛋白变体也可以从酵母或细菌中获得,以及通过重组DNA技术从转基因动物中获得。细胞外血红蛋白存在明显的局限性,即其高氧亲和力和血管内持久性不足,可以通过各种修饰来克服。游离血红蛋白的血管内半衰期可以通过分子内稳定、与大分子连接、分子间交联(多聚血红蛋白溶液)或微囊化而显著延长。人血红蛋白的氧亲和力可以通过将变构调节剂偶联到2,3-二磷酸甘油酸位点来降低,例如磷酸吡哆醛,而牛血红蛋白的氧亲和力本来就低。目前,人磷酸吡哆醛化多聚血红蛋白溶液和牛多聚血红蛋白溶液至少满足了作为氧运输血浆代用品的3个主要要求中的2个,即维持循环血容量并提供额外可利用的氧容量。然而,所有血红蛋白制剂都存在令人担忧的潜在血管收缩作用和肾毒性问题。不过,目前工业界和研究小组正在做出重大努力,有理由希望在可预见的未来实现改良血红蛋白溶液作为氧载体的概念。

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