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III型抗冻蛋白与人唾液酸合酶类抗冻结构域的主链动力学比较。

Comparison of backbone dynamics of the type III antifreeze protein and antifreeze-like domain of human sialic acid synthase.

作者信息

Choi Yong-Geun, Park Chin-Ju, Kim Hee-Eun, Seo Yeo-Jin, Lee Ae-Ree, Choi Seo-Ree, Lee Shim Sung, Lee Joon-Hwa

机构信息

Department of Chemistry and Research Institute of Natural Science, Gyeongsang National University, Jinju, Gyeongnam, 660-701, Republic of Korea.

出版信息

J Biomol NMR. 2015 Feb;61(2):137-50. doi: 10.1007/s10858-014-9895-2. Epub 2015 Jan 10.

DOI:10.1007/s10858-014-9895-2
PMID:25575834
Abstract

Antifreeze proteins (AFPs) are found in a variety of cold-adapted (psychrophilic) organisms to promote survival at subzero temperatures by binding to ice crystals and decreasing the freezing temperature of body fluids. The type III AFPs are small globular proteins that consist of one α-helix, three 3(10)-helices, and two β-strands. Sialic acids play important roles in a variety of biological functions, such as development, recognition, and cell adhesion and are synthesized by conserved enzymatic pathways that include sialic acid synthase (SAS). SAS consists of an N-terminal catalytic domain and a C-terminal antifreeze-like (AFL) domain, which is similar to the type III AFPs. Despite having very similar structures, AFL and the type III AFPs exhibit very different temperature-dependent stability and activity. In this study, we have performed backbone dynamics analyses of a type III AFP (HPLC12 isoform) and the AFL domain of human SAS (hAFL) at various temperatures. We also characterized the structural/dynamic properties of the ice-binding surfaces by analyzing the temperature gradient of the amide proton chemical shift and its correlation with chemical shift deviation from random coil. The dynamic properties of the two proteins were very different from each other. While HPLC12 was mostly rigid with a few residues exhibiting slow motions, hAFL showed fast internal motions at low temperature. Our results provide insight into the molecular basis of thermostability and structural flexibility in homologous psychrophilic HPLC12 and mesophilic hAFL proteins.

摘要

抗冻蛋白(AFPs)存在于多种适应寒冷(嗜冷)的生物体中,通过与冰晶结合并降低体液的冰点来促进在零下温度下的生存。III型抗冻蛋白是由一个α螺旋、三个3(10)螺旋和两条β链组成的小球形蛋白质。唾液酸在多种生物学功能中发挥重要作用,如发育、识别和细胞黏附,并且由包括唾液酸合酶(SAS)在内的保守酶促途径合成。SAS由一个N端催化结构域和一个C端抗冻样(AFL)结构域组成,该结构域与III型抗冻蛋白相似。尽管结构非常相似,但AFL和III型抗冻蛋白表现出非常不同的温度依赖性稳定性和活性。在本研究中,我们对III型抗冻蛋白(HPLC12亚型)和人SAS的AFL结构域(hAFL)在不同温度下进行了主链动力学分析。我们还通过分析酰胺质子化学位移的温度梯度及其与随机卷曲化学位移偏差的相关性,表征了冰结合表面的结构/动力学性质。这两种蛋白质的动力学性质彼此非常不同。虽然HPLC12大多刚性,只有少数残基表现出缓慢运动,但hAFL在低温下表现出快速的内部运动。我们的结果为同源嗜冷HPLC12和嗜温hAFL蛋白的热稳定性和结构灵活性的分子基础提供了见解。

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本文引用的文献

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J Biomol NMR. 2013 Feb;55(2):225-30. doi: 10.1007/s10858-012-9703-9. Epub 2013 Jan 4.
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Engineering a naturally inactive isoform of type III antifreeze protein into one that can stop the growth of ice.将天然无活性的 III 型抗冻蛋白同工型工程化为能够阻止冰生长的形式。
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用于生产脊椎动物重组唾液酸转移酶的中国仓鼠卵巢细胞工程。
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