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Mito-nuclear co-evolution: the positive and negative sides of functional ancient mutations

机译:线粒体核共同进化:功能性古代突变的正反两面

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摘要

Most cell functions are carried out by interacting factors, thus underlying the functional importance of genetic interactions between genes, termed epistasis. Epistasis could be under strong selective pressures especially in conditions where the mutation rate of one of the interacting partners notably differs from the other. Accordingly, the order of magnitude higher mitochondrial DNA (mtDNA) mutation rate as compared to the nuclear DNA (nDNA) of all tested animals, should influence systems involving mitochondrial-nuclear (mito-nuclear) interactions. Such is the case of the energy producing oxidative phosphorylation (OXPHOS) and mitochondrial translational machineries which are comprised of factors encoded by both the mtDNA and the nDNA. Additionally, the mitochondrial RNA transcription and mtDNA replication systems are operated by nDNA-encoded proteins that bind mtDNA regulatory elements. As these systems are central to cell life there is strong selection toward mito-nuclear co-evolution to maintain their function. However, it is unclear whether (A) mito-nuclear co-evolution befalls only to retain mitochondrial functions during evolution or, also, (B) serves as an adaptive tool to adjust for the evolving energetic demands as species’ complexity increases. As the first step to answer these questions we discuss evidence of both negative and adaptive (positive) selection acting on the mtDNA and nDNA-encoded genes and the effect of both types of selection on mito-nuclear interacting factors. Emphasis is given to the crucial role of recurrent ancient (nodal) mutations in such selective events. We apply this point-of-view to the three available types of mito-nuclear co-evolution: protein–protein (within the OXPHOS system), protein-RNA (mainly within the mitochondrial ribosome), and protein-DNA (at the mitochondrial replication and transcription machineries).
机译:大多数细胞功能是由相互作用的因子来完成的,因此潜在的基因之间的基因相互作用的功能重要性,称为上位性。上位性可能处于较强的选择压力下,尤其是在其中一个相互作用伴侣的突变率与另一个相互作用伴侣的突变率明显不同的情况下。因此,与所有测试动物的核DNA(nDNA)相比,线粒体DNA(mtDNA)突变率高一个数量级,这应该会影响涉及线粒体-核(mito-nuclear)相互作用的系统。产生能量的氧化磷酸化(OXPHOS)和线粒体翻译机制就是这种情况,它们由mtDNA和nDNA编码的因子组成。此外,线粒体RNA转录和mtDNA复制系统由结合mtDNA调控元件的nDNA编码蛋白操纵。由于这些系统对于细胞生命至关重要,因此有很多选择来维持细胞核的功能,以进行微核共同进化。但是,目前尚不清楚(A)线粒体-核共同进化是否仅在进化过程中保留了线粒体功能而下降,或者(B)还是一种适应工具,可随着物种的复杂性增加而适应不断发展的能量需求。作为回答这些问题的第一步,我们讨论了对mtDNA和nDNA编码的基因起作用的阴性和自适应(阳性)选择的证据,以及两种选择对微核相互作用因子的影响。强调了反复发生的古代(结节)突变在此类选择性事件中的关键作用。我们将这种观点应用于线粒体-核共进化的三种可用类型:蛋白质-蛋白质(在OXPHOS系统内),蛋白质-RNA(主要在线粒体核糖体内)和蛋白质-DNA(在线粒体中)复制和转录机制)。

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