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The Rieske Protein: A Case Study on the Pitfalls of Multiple Sequence Alignments and Phylogenetic Reconstruction

机译:Rieske蛋白:多个序列比对和系统发育重建的陷阱的案例研究

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摘要

Previously published phylogenetic trees reconstructed on “Rieske protein” sequences frequently are at odds with each other, with those of other subunits of the parent enzymes and with small-subunit rRNA trees. These differences are shown to be at least partially if not completely due to problems in the reconstruction procedures. A major source of erroneous Rieske protein trees lies in the presence of a large, poorly conserved domain prone to accommodate very long insertions in well-defined structural hot spots substantially hampering multiple alignments. The remaining smaller domain, in contrast, is too conserved to allow distant phylogenies to be deduced with sufficient confidence. Three-dimensional structures of representatives from this protein family are now available from phylogenetically distant species and from diverse enzymes. Multiple alignments can thus be refined on the basis of these structures. We show that structurally guided alignments of Rieske proteins from Rieske–cytochrome b complexes and arsenite oxidases strongly reduce conflicts between resulting trees and those obtained on their companion enzyme subunits. Further problems encountered during this work, mainly consisting in database errors such as wrong annotations and frameshifts, are described. The obtained results are discussed against the background of hypotheses stipulating pervasive lateral gene transfer in prokaryotes.
机译:先前发表的以“ Rieske蛋白”序列重建的系统发育树经常相互矛盾,与亲本酶其他亚基的树和小亚基rRNA树也相互矛盾。这些差异显示为至少部分(如果不是完全的话)是由于重建程序中的问题。错误的Rieske蛋白树的主要来源在于存在大的,保守性差的结构域,该结构域倾向于在定义良好的结构热点中容纳很长的插入,从而严重阻碍了多重比对。相反,其余较小的域过于保守,无法以足够的置信度推导远处的系统发育。现在可以从系统发育远缘的物种和多种酶中获得该蛋白质家族代表的三维结构。因此,可以在这些结构的基础上完善多重比对。我们显示,从Rieske-细胞色素b复合物和亚砷酸氧化酶出发的Rieske蛋白的结构指导比对可大大减少所得树木与在其同伴酶亚基上获得的树木之间的冲突。描述了在这项工作中遇到的其他问题,主要是数据库错误,例如错误的注释和移码。在规定原核生物普遍进行侧向基因转移的假设的背景下讨论了获得的结果。

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