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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Characterization of the deoxyhemoglobin binding site on human erythrocyte band 3: implications for O2 regulation of erythrocyte properties.
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Characterization of the deoxyhemoglobin binding site on human erythrocyte band 3: implications for O2 regulation of erythrocyte properties.

机译:人红细胞带上脱氧血红蛋白结合位点的表征3:对O2调节红细胞特性的影响。

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摘要

Band 3, the major protein of the human erythrocyte membrane, associates with multiple metabolic, ion transport, and structural proteins. Functional studies demonstrate that the oxygenation state of the erythrocyte regulates cellular properties performed by these and/or related proteins. Because deoxyhemoglobin, but not oxyhemoglobin, binds band 3 reversibly with high affinity, these observations raise the hypothesis that hemoglobin might regulate erythrocyte properties through its reversible, oxygenation-dependent association with band 3. To explore this hypothesis, we have characterized the binding site of deoxyHb on human erythrocyte band 3. We report that (1) deoxyHb binds to residues 12-23 of band 3; (2) mutation of residues on either side of this sequence greatly enhances affinity of deoxyHb for band 3, suggesting that evolution of a higher affinity interaction would have been possible had it been beneficial for survival; (3) Hb does not bind to 2 other sequences in band 3 despite their high sequence homology to residues 12-23, and (4) the Hb binding site on band 3 lies proximal to binding sites for glycolytic enzymes, band 4.1 and ankyrin, suggesting possible mechanisms through which multifarious erythrocyte properties might be regulated by the oxygenation state of the cell.
机译:带3是人类红细胞膜的主要蛋白质,与多种代谢,离子转运和结构蛋白相关。功能研究表明,红细胞的氧合状态调节了这些和/或相关蛋白的细胞特性。由于脱氧血红蛋白(而非氧合血红蛋白)以高亲和力可逆地结合3带,因此,这些观察提出了这样的假设,即血红蛋白可能通过与带3的可逆的,氧合依赖性的结合来调节红细胞的性质。为探索这一假设,我们已经表征了人类红细胞3带上的脱氧Hb。我们报道(1)脱氧Hb与3带的12-23残基结合; (2)该序列任一侧残基的突变大大增强了脱氧Hb对3带的亲和力,表明如果对存活有益,则可能发展出更高亲和力的相互作用。 (3)尽管Hb与残基12-23具有很高的序列同源性,但Hb并未与3带中的其他2个序列结合,并且(4)3带中的Hb结合位点位于糖酵解酶的结合位点附近,即4.1带和锚蛋白。提示可能的机制,通过这些机制可能通过细胞的氧合状态调节多种红细胞特性。

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