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首页> 外文期刊>Proteins: Structure, Function, and Genetics >Modeling the third loop of short-chain snake venom neurotoxins: roles of the short-range and long-range interactions.
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Modeling the third loop of short-chain snake venom neurotoxins: roles of the short-range and long-range interactions.

机译:建模短链蛇毒神经毒素的第三环:短程和长程相互作用的作用。

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摘要

The influence of long-range interactions on local structures is an important issue in understanding protein folding process and protein structure stability. Using short-chain snake venom neurotoxin as a model system, we have studied the conformational properties of eight different loop III sequences either in the environment of one of the short-chain neurotoxin, erabutoxin b (PDB ID 1nxb), or in free state by Monte Carlo simulated annealing method. The surrounding protein structure was found to be crucial in stabilizing the loop conformation. Although all the eight peptides prefer type V beta turn in solution, three of them (KPGI, KPGV, KSGI) turn to type II beta turn and the other five (KKGI, KKGV, KNGI, KQGI, and KRGV) are confined to more rigid type V beta turn conformation in the protein structure. Using flexible tetra-glycine-peptide to screen the backbone conformational space in the protein environment also validates the results. This study shows that long-range interactions do contribute to the stability and the types of conformation for a surface loop in protein, while short-range interactions may only provide candidate conformations, which then have to be filtered by the long-range interactions further.
机译:远程相互作用对局部结构的影响是理解蛋白质折叠过程和蛋白质结构稳定性的重要问题。以短链蛇毒神经毒素为模型系统,我们研究了短链神经毒素erabutoxin b(PDB ID 1nxb)之一在游离状态下的八个环III序列的构象特性。蒙特卡洛模拟退火方法。发现周围的蛋白质结构对于稳定环构象至关重要。尽管所有八种肽都倾向于在溶液中使用V型β转体,但其中三种(KPGI,KPGV,KSGI)转为II型β转体,而其他五种(KKGI,KKGV,KNGI,KQGI和KRGV)被限制为更严格蛋白质结构中的V型β转弯构象。使用柔性的四甘氨酸肽在蛋白质环境中筛选主链构象空间也可以验证结果。这项研究表明,长距离相互作用确实有助于蛋白质中表面环的稳定性和构象类型,而短距离相互作用可能仅提供候选构象,然后必须通过长距离相互作用进一步过滤掉。

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