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葡聚糖-苯六羧酸的共价标记对血红蛋白的影响。

Effect of covalent labeling of dextran-benzenehexacarboxylate on hemoglobin.

作者信息

Sacco D, Dellacherie E, Prouchayret F

机构信息

Laboratory of Macromolecular Physical Chemistry, URA-CNRS-494, ENSIC, Nancy, France.

出版信息

J Protein Chem. 1994 Jan;13(1):1-8. doi: 10.1007/BF01891986.

Abstract

The covalent fixation of benzenehexacarboxylate (BHC) onto dextran was carried out according to several reaction schemes. The polyanionic polymers thus synthesized were capable of decreasing the oxygen affinity of hemoglobin by specifically interacting with the 2,3-diphosphoglycerate (2,3-DPG) binding site of the protein. The intensity of this effect was correlated to both the chemical structure of the polyanionic polymers and the BHC content in polymer. The polyanionic polymer, containing 0.035 mol BHC/g and presenting no cross-linking between its polymer chains, possessed the best effector properties. These properties were used to direct the covalent fixation of the dextran-benzenehexacarboxylate onto the phosphate binding site of the protein. The resulting hemoglobin was mainly substituted at the same time by one or more linked BHC onto both alpha beta dimers in the vicinity of the 2,3-DPG site. Thus, the modification of hemoglobin led to an increase in the hydrodynamic volume of each dimer sufficient to limit the diffusion of the conjugates through the kidney membrane, even if the conjugates had dissociated into alpha beta dimers. Compared to that of free hemoglobin, the oxygen affinity of the conjugates was significantly decreased. This type of covalent conjugate exhibited general properties quite suitable for use as blood substitutes.

摘要

根据几种反应方案,将苯六羧酸盐(BHC)共价固定在葡聚糖上。由此合成的聚阴离子聚合物能够通过与蛋白质的2,3-二磷酸甘油酸(2,3-DPG)结合位点特异性相互作用来降低血红蛋白的氧亲和力。这种效应的强度与聚阴离子聚合物的化学结构和聚合物中的BHC含量相关。含有0.035 mol BHC/g且聚合物链之间不存在交联的聚阴离子聚合物具有最佳的效应特性。这些特性被用于将葡聚糖-苯六羧酸盐共价固定在蛋白质的磷酸盐结合位点上。所得的血红蛋白主要同时在2,3-DPG位点附近的αβ二聚体上被一个或多个连接的BHC取代。因此,血红蛋白的修饰导致每个二聚体的流体力学体积增加,足以限制缀合物通过肾膜的扩散,即使缀合物已解离成αβ二聚体。与游离血红蛋白相比,缀合物的氧亲和力显著降低。这种类型的共价缀合物表现出非常适合用作血液替代品的一般特性。

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