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RET和各向异性测量确定了泪液脂质运载蛋白中保守的色氨酸17与异亮氨酸98和苯丙氨酸99的接近程度。

RET and anisotropy measurements establish the proximity of the conserved Trp17 to Ile98 and Phe99 of tear lipocalin.

作者信息

Gasymov Oktay K, Abduragimov Adil R, Yusifov Taleh N, Glasgow Ben J

机构信息

Department of Pathology, School of Medicine, University of California at Los Angeles, Los Angeles, CA 90095, USA.

出版信息

Biochemistry. 2002 Jul 16;41(28):8837-48. doi: 10.1021/bi0121003.

Abstract

Previous studies suggest that the conserved Trp17 on strand A of TL has a role in lipocalin stability and interacts, directly or indirectly, with Ile98 and Phe99 on strand G to influence ligand binding. Here, we determined the proximity of Trp17 to Ile98 and Phe99. Time-resolved fluorescence experiments showed resonance energy transfer between tryptophans at positions 17 and 98. In addition, an exciton effect was discovered in CD experiments resulting from interactions of the excited states of these tryptophans. Fluorescence anisotropy values of mutants containing two tryptophans (positions 99/17 and 98/17) were lower than expected in the absence of RET, confirming that these residues are proximate in tear lipocalin. The data support a model of tear lipocalin in which Trp17 and Phe99 are close together deep in the cavity and participate in an internal hydrophobic cluster. Ile98 is proximate to Trp17 but faces toward the outside of the cavity and in the model is part of an external hydrophobic patch. Comparison with beta-lactoglobulin suggests that these motifs may have an important influence on protein stability and ligand binding in other members of the lipocalin family.

摘要

先前的研究表明,泪液脂质运载蛋白(TL)A链上保守的色氨酸17(Trp17)在脂质运载蛋白稳定性方面发挥作用,并直接或间接地与G链上的异亮氨酸98(Ile98)和苯丙氨酸99(Phe99)相互作用,从而影响配体结合。在此,我们确定了Trp17与Ile98和Phe99之间的距离。时间分辨荧光实验显示,17位和98位色氨酸之间存在共振能量转移。此外,在圆二色性实验中发现了一种激子效应,该效应源于这些色氨酸激发态之间的相互作用。含有两个色氨酸(99/17位和98/17位)的突变体的荧光各向异性值低于在不存在共振能量转移(RET)时的预期值,这证实了这些残基在泪液脂质运载蛋白中位置相近。这些数据支持了一种泪液脂质运载蛋白模型,其中Trp17和Phe99在腔的深处靠在一起,并参与一个内部疏水簇。Ile98与Trp17位置相近,但面向腔的外部,在该模型中是外部疏水斑块的一部分。与β-乳球蛋白的比较表明,这些基序可能对脂质运载蛋白家族其他成员的蛋白质稳定性和配体结合有重要影响。

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