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牛α-乳白蛋白的脂质结合特异性:一种多维方法。

Lipid binding specificity of bovine α-lactalbumin: a multidimensional approach.

作者信息

Chaudhuri Arunima, Chattopadhyay Amitabha

机构信息

CSIR-Centre for Cellular and Molecular Biology, Uppal Road, Hyderabad 500 007, India.

CSIR-Centre for Cellular and Molecular Biology, Uppal Road, Hyderabad 500 007, India.

出版信息

Biochim Biophys Acta. 2014 Aug;1838(8):2078-86. doi: 10.1016/j.bbamem.2014.04.027. Epub 2014 May 4.

DOI:10.1016/j.bbamem.2014.04.027
PMID:24802274
Abstract

Many soluble proteins are known to interact with membranes in partially disordered states, and the mechanism and relevance of such interactions in cellular processes are beginning to be understood. Bovine α-lactalbumin (BLA) represents an excellent prototype for monitoring membrane interaction due to its conformational plasticity. In this work, we comprehensively monitored the interaction of apo-BLA with zwitterionic and negatively charged membranes utilizing a variety of approaches. We show that BLA preferentially binds to negatively charged membranes at acidic pH with higher binding affinity. This is supported by spectral changes observed with a potential-sensitive membrane probe and fluorescence anisotropy measurements of a hydrophobic probe. Our results show that BLA exhibits a molten globule conformation when bound to negatively charged membranes. We further show, using the parallax approach, that BLA penetrates the interior of negatively charged membranes, and tryptophan residues are localized at the membrane interface. Red edge excitation shift (REES) measurements reveal that the immediate environment of tryptophans in membrane-bound BLA is restricted, and the restriction is dependent on membrane lipid composition. We envision that understanding the mechanism of BLA-membrane interaction would help in bioengineering of α-lactalbumin, and to address the mechanism of tumoricidal and antimicrobial activities of BLA-oleic acid complex.

摘要

许多可溶性蛋白质已知会以部分无序状态与膜相互作用,并且这种相互作用在细胞过程中的机制和相关性正开始被理解。由于其构象可塑性,牛α-乳白蛋白(BLA)是监测膜相互作用的一个出色原型。在这项工作中,我们利用多种方法全面监测了脱辅基BLA与两性离子膜和带负电荷膜的相互作用。我们表明,在酸性pH下,BLA优先以更高的结合亲和力与带负电荷的膜结合。这得到了用电位敏感膜探针观察到的光谱变化以及疏水探针的荧光各向异性测量的支持。我们的结果表明,BLA与带负电荷的膜结合时呈现熔球构象。我们进一步使用视差方法表明,BLA穿透带负电荷膜的内部,并且色氨酸残基位于膜界面处。红边激发位移(REES)测量表明,膜结合的BLA中色氨酸的紧邻环境受到限制,并且这种限制取决于膜脂质组成。我们设想,了解BLA与膜相互作用的机制将有助于α-乳白蛋白的生物工程,并有助于阐明BLA-油酸复合物的杀肿瘤和抗菌活性机制。

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