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通过定点色氨酸荧光研究泪液载脂蛋白 pH 依赖性构象变化。

pH-Dependent conformational changes in tear lipocalin by site-directed tryptophan fluorescence.

机构信息

Department of Pathology, UCLA School of Medicine, Jules Stein Eye Institute, 100 Stein Plaza, Los Angeles, California 90095, USA.

出版信息

Biochemistry. 2010 Jan 26;49(3):582-90. doi: 10.1021/bi901435q.

Abstract

Tear lipocalin (TL), a major protein of human tears, binds a broad array of endogenous ligands. pH-dependent ligand binding in TL may have functional implications in tears. Previously, conformational selections of the AB and GH loops have been implicated in ligand binding by site-directed tryptophan fluorescence (SDTF). In this study, SDTF was applied to the AB and GH loops to investigate pH-driven conformational changes relevant to ligand binding. Both loops demonstrate significant but distinct conformational rearrangements over a wide pH range. In the low-pH transition, from 7.3 to 3.0, residues of the GH loop exhibit decreased solvent accessibilities. In acrylamide quenching experiments, the average quenching rate constant (k(q), accessibility parameter) of the residues in the GH loop is decreased approximately 38%, from 2.1 x 10(9) to 1.3 x 10(9) M(-1) s(-1). However, despite the significant changes in accessibilities for some residues in the AB loop, the average accessibility per residue remained unchanged (average k(q) = 1.2 M(-1) s(-1)). Accordingly, the low-pH transition induces conformational changes that reshuffle the accessibility profiles of the residues in the AB loop. A significant difference in the titration curves between the holo and apo forms of the W28 mutant suggests that the protonation states of the residues around position 28 modulate conformational switches of the AB loop relevant to ligand binding.

摘要

泪液脂质运载蛋白(TL)是人类泪液中的主要蛋白质,可结合广泛的内源性配体。TL 中 pH 依赖性配体结合可能对泪液具有功能意义。先前,通过定点色氨酸荧光(SDTF)已证实 AB 和 GH 环的构象选择参与配体结合。在这项研究中,应用 SDTF 研究 AB 和 GH 环,以研究与配体结合相关的 pH 驱动的构象变化。在很宽的 pH 范围内,两个环都显示出显著但不同的构象重排。在从 7.3 到 3.0 的低 pH 转变中,GH 环的残基显示出溶剂可及性降低。在丙烯酰胺猝灭实验中,GH 环中残基的平均猝灭速率常数(k(q),可及性参数)降低了约 38%,从 2.1 x 10(9)降至 1.3 x 10(9) M(-1) s(-1)。然而,尽管 AB 环中一些残基的可及性发生了显著变化,但每个残基的平均可及性保持不变(平均 k(q) = 1.2 M(-1) s(-1))。因此,低 pH 转变诱导了重新排列 AB 环中残基可及性分布的构象变化。W28 突变体的全酶和apo 形式之间的滴定曲线存在显著差异,表明位置 28 周围残基的质子化状态调节与配体结合相关的 AB 环的构象开关。

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