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苯乙二醛对带3蛋白介导的阴离子跨红细胞膜转运的三种不同作用。

Three different actions of phenylglyoxal on band 3 protein-mediated anion transport across the red blood cell membrane.

作者信息

Gärtner E M, Liebold K, Legrum B, Fasold H, Passow H

机构信息

Max Planck Institut für Biophysik, Frankfurt am Main, Germany.

出版信息

Biochim Biophys Acta. 1997 Jan 31;1323(2):208-22. doi: 10.1016/s0005-2736(96)00187-3.

Abstract

Phenylglyoxalation of the red blood cell membrane leads to three superimposed effects on band 3 protein-mediated anion equilibrium exchange as measured by means of radiosulfate: (1) a shift of the curve relating transport activity to pH towards lower pH values, possibly in combination with an increase of the maximal transport activity. This is accompanied by effect (2), the abolishment of a chloride-stimulated component of anion transport seen at low pH values. Effect (3) consists of inhibition of anion equilibrium exchange. Effect (1) prevails when phenylglyoxalation is performed at low concentrations of PG and low pH, while effect (3) predominates when exposure to PG is executed at high pH and high concentration of PG. Effect (1) is associated with a decrease of the Ki values for inhibition and binding of the reversibly acting stilbene disulfonates DNDS and DBDS. The inhibition observed as a consequence of effect (3) is linearly related to a decrease of the capacity of band 3 to combine with the stilbene disulfonate DBDS. The results are interpreted on the assumption that PG is capable of reacting with two or possibly three distinct binding sites in band 3. Reaction with one of them leads to effect (1) and, perhaps, to effect (2); reaction with the other to effect (3). The latter is possibly due to modification of Arg 730, which is homologous to Arg 748 in mouse band 3. Site-directed mutagenesis of this arginine residue showed that it is required for band 3-mediated anion transport.

摘要

红细胞膜的苯乙二醛化对通过放射性硫酸盐测量的带3蛋白介导的阴离子平衡交换产生三种叠加效应:(1)将与转运活性相关的曲线向较低pH值移动,可能与最大转运活性增加相结合。这伴随着效应(2),即在低pH值下观察到的氯离子刺激的阴离子转运成分的消除。效应(3)包括对阴离子平衡交换的抑制。当在低浓度的苯乙二醛和低pH值下进行苯乙二醛化时,效应(1)占主导,而当在高pH值和高浓度的苯乙二醛下进行暴露时,效应(3)占主导。效应(1)与可逆作用的芪二磺酸盐DNDS和DBDS的抑制和结合的Ki值降低有关。由于效应(3)观察到的抑制与带3与芪二磺酸盐DBDS结合能力的降低呈线性相关。这些结果是基于苯乙二醛能够与带3中的两个或可能三个不同结合位点反应的假设来解释的。与其中一个位点反应导致效应(1),也许还导致效应(2);与另一个位点反应导致效应(3)。后者可能是由于精氨酸730的修饰,它与小鼠带3中的精氨酸748同源。对这个精氨酸残基进行定点诱变表明,它是带3介导的阴离子转运所必需的。

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