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以白蛋白-血红素进行交换输血作为对麻醉大鼠的人工输氧:生理反应、氧输送以及红细胞对氧化血红素位点的减少作用

Exchange transfusion with albumin-heme as an artificial O2-infusion into anesthetized rats: physiological responses, O2-delivery, and reduction of the oxidized hemin sites by red blood cells.

作者信息

Tsuchida E, Komatsu T, Hamamatsu K, Matsukawa Y, Tajima A, Yoshizu A, Izumi Y, Kobayashi K

机构信息

Department of Polymer Chemistry, Advanced Research Institute for Science & Engineering, Waseda University, Tokyo 169-8555, Japan.

出版信息

Bioconjug Chem. 2000 Jan-Feb;11(1):46-50. doi: 10.1021/bc990065v.

Abstract

Human serum albumin (HSA) incorporating synthetic hemes, the tetrakis(o-pivalamido)phenylporphinatoiron(II) derivative (FeP), is an artificial hemoprotein (HSA-FeP) which is able to reversibly bind and release dioxygen under physiological conditions (in aqueous media, pH 7.4, 37 degrees C) like hemoglobin and myoglobin. Physiological responses to exchange transfusion with HSA-FeP solution [[HSA], 5 g/dL; FeP/HSA, 4 (mol/mol)] into rats after hemodilution and hemorrhage (Hct, about 10%) has been evaluated. The declined mean arterial pressure (MAP) and blood flow after a 70% exchange with HSA and the further 40% bleeding of blood were significantly recovered up to about 90% of the baseline values by the injection of HSA-FeP. Furthermore, the renal cortical O(2)-tensions and skeletal tissue O(2)-tensions were also increased, indicating the in vivo O(2)-delivery of HSA-FeP. Autoxidation of ferrous Fe(II)P to ferric Fe(III)P was retarded in the blood stream; the half-lifetime of the dioxygenated FeP [tau(1/2)(O(2))] in vivo was 4.1 h [cf. 1.0 h (in vitro)]. It has been found that autooxidized Fe(III)P was certainly reduced in the whole blood suspension. Physiological concentrations of ascorbic acid continuously provided by red blood cells probably rereduces Fe(III)P, leading to the apparent long lifetime of the dioxygenated species of FeP.

摘要

结合合成血红素的人血清白蛋白(HSA),即四(邻新戊酰胺基)苯基卟啉铁(II)衍生物(FeP),是一种人工血红蛋白(HSA-FeP),它能够在生理条件下(在水介质中,pH 7.4,37℃)像血红蛋白和肌红蛋白一样可逆地结合和释放双氧。已经评估了在血液稀释和出血(红细胞压积约10%)后向大鼠输注HSA-FeP溶液[[HSA],5 g/dL;FeP/HSA,4(摩尔/摩尔)]进行交换输血的生理反应。在使用HSA进行70%的交换以及进一步40%的放血后下降的平均动脉压(MAP)和血流,通过注射HSA-FeP显著恢复至基线值的约90%。此外,肾皮质O₂张力和骨骼肌组织O₂张力也增加,表明HSA-FeP在体内具有氧输送能力。亚铁Fe(II)P在血流中向高铁Fe(III)P的自氧化受到抑制;体内双氧合FeP的半衰期[τ₁/₂(O₂)]为4.1小时[参考1.0小时(体外)]。已经发现全血悬浮液中自氧化的Fe(III)P确实被还原。红细胞持续提供的生理浓度的抗坏血酸可能将Fe(III)P再次还原,导致FeP双氧合物种的明显长寿命。

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