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Band 3 蛋白的构象动力学:对红细胞衰老信号的意义。

Large conformational dynamics in Band 3 protein: Significance for erythrocyte senescence signalling.

机构信息

Department of Biochemistry, Membrane Protein Disease Research Group, University of Alberta, Edmonton, Alberta T6G 2H7, Canada.

Department of Biochemistry, Membrane Protein Disease Research Group, University of Alberta, Edmonton, Alberta T6G 2H7, Canada.

出版信息

Biochim Biophys Acta Biomembr. 2021 Oct 1;1863(10):183678. doi: 10.1016/j.bbamem.2021.183678. Epub 2021 Jun 24.

DOI:10.1016/j.bbamem.2021.183678
PMID:34175296
Abstract

Band 3 (Anion Exchanger 1, AE1), the predominant protein of erythrocyte membranes, facilitates Cl/HCO exchange and anchors the plasma membrane to the cytoskeleton. The Band 3 crystal structure revealed the amino acid 812-830 region as intracellular, conflicting with protein chemical data that suggested extracellular disposition. Further, circulating senescent cell auto-antibody that cannot enter erythrocytes, binds two regions of Band 3: residues 538-554 and 812-830. To reconcile this discrepancy, we assessed localization of residues 812-830 with Band 3 expressed in HEK293 cells and human erythrocytes, using chemical labeling probes and an antibody against residues 812-830. Antibody and chemical probes revealed reorientation of 812-830 region between extracellular and intracellular. This dramatic conformational change is an intrinsic property of the Band 3 molecule, occurring when expressed in HEK293 cells and without the damage that occurs during erythrocyte circulation. Conditions used to crystallize Band 3 for structural determination did not alter conformational dynamics. Collectively, these data reveal large Band 3 conformational dynamics localized to a region previously identified as an erythrocyte senescence epitope. Surface exposure of the senescence epitope (812-830), limited by conformational dynamics, may act as the "molecular clock" in erythrocyte senescence.

摘要

Band 3(阴离子交换器 1,AE1)是红细胞膜的主要蛋白,促进 Cl/HCO 交换,并将质膜锚定到细胞骨架上。Band 3 的晶体结构揭示了氨基酸 812-830 区域是细胞内的,与表明细胞外分布的蛋白质化学数据相矛盾。此外,不能进入红细胞的循环衰老细胞自身抗体结合 Band 3 的两个区域:残基 538-554 和 812-830。为了解决这一差异,我们使用化学标记探针和针对残基 812-830 的抗体,评估了在 HEK293 细胞和人红细胞中表达的 Band 3 中残基 812-830 的定位。抗体和化学探针揭示了 812-830 区域在细胞外和细胞内之间的重新定向。这种剧烈的构象变化是 Band 3 分子的固有特性,当在 HEK293 细胞中表达时会发生,而无需在红细胞循环过程中发生损伤。用于确定 Band 3 结构的结晶条件并未改变构象动力学。总之,这些数据揭示了定位于先前鉴定为红细胞衰老表位的区域的大量 Band 3 构象动力学。衰老表位(812-830)的表面暴露受构象动力学限制,可能作为红细胞衰老的“分子钟”。

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