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Structural test of the parameterized-backbone method for protein design

机译:参数化骨干蛋白设计方法的结构测试

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Designing new protein folds requires a method for simultaneously optimizing the conformation of the backbone and the side-chains. One approach to this problem is the use of a parameterized backbone, which allows the systematic exploration of families of structures. We report the crystal structure of RH3, a right-handed, three-helix coiled coil that was designed using a parameterized backbone and detailed modeling of core packing. This crystal structure was determined using another rationally designed feature, a metal-binding site that permitted experimental phasing of the X-ray data. RH3 adopted the intended fold, which has not been observed previously in biological proteins. Unanticipated structural asymmetry in the trimer was a principal source of variation within the RH3 structure. The sequence of RH3 differs from that of a previously characterized right-handed tetramer, RH4, at only one position in each 11 amino acid sequence repeat. This close similarity indicates that the design method is sensitive to the core packing interactions that specify the protein structure. Comparison of the structures of RH3 and RH4 indicates that both steric overlap and cavity formation provide strong driving forces for oligomer specificity. (C) 2004 Elsevier Ltd. All rights reserved.
机译:设计新的蛋白质折叠需要同时优化主链和侧链构象的方法。解决此问题的一种方法是使用参数化主干,该主干可以系统地探索结构族。我们报告了RH3的晶体结构,这是一个右手的三螺旋盘绕线圈,该线圈使用参数化主链和核心填充的详细模型进行设计。使用另一个合理设计的特征确定了这种晶体结构,该特征是允许X射线数据进行实验定相的金属结合位点。 RH3采用了预期的折叠,这是以前在生物蛋白中尚未观察到的。三聚体中意外的结构不对称是RH3结构内变化的主要来源。 RH3的序列与先前表征的右手四聚体RH4的序列不同,在每个11个氨基酸序列重复中只有一个位置。这种紧密相似性表明设计方法对指定蛋白质结构的核心堆积相互作用敏感。 RH3和RH4的结构比较表明,空间重叠和空腔形成都为低聚物特异性提供了强大的驱动力。 (C)2004 Elsevier Ltd.保留所有权利。

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