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首页> 外文期刊>Journal of Molecular Biology >STRUCTURAL SIMILARITY BETWEEN TWO-LAYER ALPHA/BETA AND BETA-PROTEINS
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STRUCTURAL SIMILARITY BETWEEN TWO-LAYER ALPHA/BETA AND BETA-PROTEINS

机译:两层Alpha / BETA和Beta蛋白之间的结构相似性

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This paper demonstrates that overall folds of two-layer alpha/beta-proteins and beta-proteins with aligned beta-sheet packings have a number of common features. First of all, there are similar recurrent folding units, the so-called abcd-units, in proteins of both the classes. There are also some larger commonly occurring structures in many representatives of these classes. The fact that these proteins belong to different structural classes and have different functions supports the idea that some physical principles governing the polypeptide chain folding rather than the evolutionary divergence or functional convergence of proteins are the basis of such similarities. The analysis reported here shows that practically all the known protein structures of these classes can be obtained by stepwise addition of secondary structure element to the abcd-units taking into account three simple rules: (1) crossing of connection regions is prohibited; (2) alpha-helices should be packed into the alpha-layer and beta-strands in to the beta-layer of the growing structure; (3) beta alpha beta-units should be folded into right-handed superhelices; three consecutive beta-strands can be folded into the similar right-handed beta beta beta-superhelix if there is at least one additional beta-strand in the layer between the first and third ones. A possible selection of a conformation of a polypeptide chain segment by its protein environment is also discussed. [References: 90]
机译:本文证明了具有对齐的β-折叠堆积的两层α/β-蛋白质和β-蛋白质的整体折叠具有许多共同特征。首先,在这两类蛋白质中都有相似的递归折叠单元,即所谓的abcd单元。在这些类别的许多代表中,也存在一些较大的常见结构。这些蛋白质属于不同的结构类别并具有不同的功能这一事实支持以下观点:控制多肽链折叠的某些物理原理而非蛋白质的进化分歧或功能收敛是此类相似性的基础。此处报道的分析表明,考虑到三个简单的规则,可以通过将二级结构元素逐步添加到abcd单元中来获得几乎所有这些类别的已知蛋白质结构:(1)禁止交叉连接区域; (2)应该将α-螺旋堆积在生长结构的α-层中,并将β-链包裹在β-层中; (3)beta alpha beta-units应折叠为右手超螺旋;如果在第一个和第三个之间的层中至少有一个额外的beta链,则可以将三个连续的beta链折叠成类似的右手beta beta beta超螺旋。还讨论了通过其蛋白质环境对多肽链片段构象的可能选择。 [参考:90]

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