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Evolutionary assembly patterns of prokaryotic genomes

机译:原核基因组的进化装配模式

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摘要

Evolutionary innovation must occur in the context of some genomic background, which limits available evolutionary paths. For example, protein evolution by sequence substitution is constrained by epistasis between residues. In prokaryotes, evolutionary innovation frequently happens by macrogenomic events such as horizontal gene transfer (HGT). Previous work has suggested that HGT can be influenced by ancestral genomic content, yet the extent of such gene-level constraints has not yet been systematically characterized. Here, we evaluated the evolutionary impact of such constraints in prokaryotes, using probabilistic ancestral reconstructions from 634 extant prokaryotic genomes and a novel framework for detecting evolutionary constraints on HGT events. We identified 8228 directional dependencies between genes and demonstrated that many such dependencies reflect known functional relationships, including for example, evolutionary dependencies of the photosynthetic enzyme RuBisCO. Modeling all dependencies as a network, we adapted an approach from graph theory to establish chronological precedence in the acquisition of different genomic functions. Specifically, we demonstrated that specific functions tend to be gained sequentially, suggesting that evolution in prokaryotes is governed by functional assembly patterns. Finally, we showed that these dependencies are universal rather than clade-specific and are often sufficient for predicting whether or not a given ancestral genome will acquire specific genes. Combined, our results indicate that evolutionary innovation via HGT is profoundly constrained by epistasis and historical contingency, similar to the evolution of proteins and phenotypic characters, and suggest that the emergence of specific metabolic and pathological phenotypes in prokaryotes can be predictable from current genomes.
机译:进化创新必须在某些基因组背景下进行,这限制了可用的进化途径。例如,通过序列取代的蛋白质进化受到残基之间的上位性的限制。在原核生物中,进化创新经常发生在宏观基因组事件中,例如水平基因转移(HGT)。先前的工作表明,HGT可能受祖先基因组含量的影响,但尚未对这些基因水平限制的程度进行系统地表征。在这里,我们使用来自634个现存原核基因组的概率祖先重建方法和用于检测HGT事件进化限制的新颖框架,评估了这些限制在原核生物中的进化影响。我们确定了基因之间的8228个方向依赖性,并证明许多此类依赖性反映了已知的功能关系,包括例如光合酶RuBisCO的进化依赖性。通过将所有依赖关系建模为网络,我们采用了图论的方法来建立在获取不同基因组功能时的时间顺序优先顺序。具体来说,我们证明了特定的功能往往会顺序获得,这表明原核生物的进化受功能组装模式的支配。最后,我们证明了这些依赖性是通用的,而不是进化枝特异性的,并且通常足以预测给定的祖先基因组是否将获得特定的基因。综合起来,我们的结果表明,通过HGT进行的进化创新受到上位性和历史偶然性的极大限制,类似于蛋白质和表型特征的进化,并且表明原核生物中特定代谢和病理表型的出现可以从当前基因组中预测出来。

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