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When proteome meets genome: the alpha helix and the beta strand of proteins are eschewed by mRNA splice junctions and may define the minimal indivisible modules of protein architecture

机译:当蛋白质组遇到基因组时:mRNA剪接避免了蛋白质的α螺旋和β链,并可能定义了蛋白质结构的最小不可分模块

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The significance of the intron-exon structure of genes is a mystery. As eukaryotic proteins are made up of modular functional domains, each exon was suspected to encode some form of module; however, the definition of a module remained vague. Comparison of pre-mRNA splice junctions with the three-dimensional architecture of its protein product from different eukarybtes revealed that the junctions were far less likely to occur inside the α-helices and β-strands of proteins than within the more flexible linker regions ('turns' and 'loops') connecting them. The splice junctions were equally distributed in the different types of linkers and throughout the linker sequence, although a slight preference for the central region of the linker was observed. The avoidance of the α-helix and the β-strand by splice junctions suggests the existence of a selection pressure against their disruption, perhaps underscoring the investment made by nature in building these intricate secondary structures. A corollary is that the helix and the strand are the smallest integral architectural units of a protein and represent the minimal modules in the evolution of protein structure. These results should find use in comparative geno-mics, designing of cloning strategies, and in the mutual verification of genome sequences with protein structures.
机译:基因的内含子-外显子结构的重要性是一个谜。由于真核蛋白由模块功能域组成,因此每个外显子被怀疑编码某种形式的模块。但是,模块的定义仍然含糊不清。前mRNA剪接连接与来自不同真核生物的蛋白质产物的三维结构比较表明,与在更灵活的接头区域内发生连接相比,在蛋白质的α螺旋和β链内部发生这种连接的可能性要小得多(圈”和“圈”)将它们连接起来。剪接点在不同类型的接头和整个接头序列中均等分布,尽管观察到接头中心区域稍有偏爱。剪接连接避免了α-螺旋和β-链的存在,表明存在对它们破坏的选择压力,这也许强调了自然界在建造这些复杂的二级结构上的投资。一个必然的结论是,螺旋和链是蛋白质的最小整体结构单元,代表了蛋白质结构进化中的最小模块。这些结果应可用于比较基因组学,克隆策略设计以及具有蛋白质结构的基因组序列的相互验证中。

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