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HbXL99 alpha: a hemoglobin derivative that is cross-linked between the alpha subunits is useful as a blood substitute.

机译:HbXL99α:在α亚基之间交联的血红蛋白衍生物可用作血液替代物。

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摘要

Under deoxygenated conditions, bis(3,5-dibromosalicyl) fumarate reacts with hemoglobin selectively to cross-link the alpha subunits between Lys-alpha 1 99 and Lys-alpha 2 99. We have characterized further the properties of this recently described hemoglobin and have demonstrated its utility as a blood substitute. The oxygen transport characteristics of the cross-linked derivative are very similar to those of whole blood. Under physiological conditions, the partial pressure of oxygen at half-saturation of hemoglobin is increased to 29 mm Hg (1 mm Hg = 133.3 kPa), compared to 12 mm Hg for hemoglobin A, fully compensating for the absence of 2,3-bisphosphoglycerate outside of the erythrocyte. The Hill coefficient is 2.9. The dependence of the oxygen affinity of HbXL99 alpha on CO2 is also identical to that of hemoglobin A. The cross-link between the alpha subunits blocks dissociation of oxyhemoglobin into alpha beta dimers and thereby prevents renal excretion of the modified hemoglobin. In the rat, the half-life of HbXL99 alpha in plasma, at a 15% volume exchange, is increased to 3.3 hr, compared to 90 min for hemoglobin A. Cross-linking HbXL99 alpha intermolecularly with bis(sulfosuccinimidyl) suberate to form predominantly a mixture of dimers and trimers further increased the half-life of the hemoglobin within the circulation by about 2-fold. The rate of autooxidation of the transfused hemoglobin was found to be markedly reduced because of the presence of an endogenous reducing system in plasma.
机译:在脱氧条件下,富马酸双(3,5-二溴水杨基)酯与血红蛋白发生选择性反应,以使Lys-alpha 1 99和Lys-alpha 2 99之间的α亚基交联。我们进一步表征了这种最近描述的血红蛋白的性质,证明了其作为血液替代品的效用。交联衍生物的氧传输特性与全血非常相似。在生理条件下,与血红蛋白A的12 mm Hg相比,血红蛋白半饱和时的氧分压增加到29 mm Hg(1 mm Hg = 133.3 kPa),完全补偿了2,3-双磷酸甘油酯的缺失在红细胞外面。希尔系数为2.9。 HbXL99α的氧亲和力对CO2的依赖性也与血红蛋白A的依赖性相同。α亚基之间的交联会阻止氧合血红蛋白解离为αβ二聚体,从而阻止了改性血红蛋白的肾脏排泄。在大鼠中,与血红蛋白A相比,HbXL99α在血浆中的半衰期(以15%的体积交换)增加至3.3小时,而HbXL99α在分子间与辛二酸双(磺基琥珀酰亚胺基)交联形成并主要形成二聚体和三聚体的混合物进一步将血红蛋白在循环系统中的半衰期延长了约2倍。由于血浆中存在内源性还原系统,发现输血的血红蛋白的自氧化速率显着降低。

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