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Deciphering the physiological blueprint of a bacterial cell

机译:解读细菌细胞的生理蓝图

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During the last few months, several pioneer genome-wide transcriptomic, proteomic and metabolomic studies have revolutionised the understanding of bacterial biological processes, leading to a picture that resembles eukaryotic complexity. Technological advances such as next-generation high-throughput sequencing and high-density oligonucleotide microarrays have allowed the determination, in several bacteria, of the entire boundaries of all expressed transcripts. Consequently, novel RNA-mediated regulatory mechanisms have been discovered including multifunctional RNAs. Moreover, resolution of bacterial proteome organisation (interactome) and global protein localisation (localizome) have unveiled an unanticipated complexity that highlights the significance of protein multifunctionality and localisation in the cell. Also, analysis of a complete bacterial metabolic network has again revealed a high fraction of multifunctional enzymes and an unexpectedly high level of metabolic responses and adaptation. Altogether, these novel approaches have permitted the deciphering of the entire physiological landscape of one of the smallest bacteria, Mycoplasma pneumoniae. Here, we summarise and discuss recent findings aimed at defining the blueprint of any prokaryote.
机译:在过去的几个月中,几项开拓性的全基因组转录组,蛋白质组学和代谢组学研究彻底改变了对细菌生物学过程的理解,从而形成了一种类似于真核生物复杂性的图景。诸如下一代高通量测序和高密度寡核苷酸微阵列等技术进步,使得可以在几种细菌中确定所有表达的转录本的整个边界。因此,已经发现了新型的RNA介导的调节机制,包括多功能RNA。此外,细菌蛋白质组学组织(相互作用组)和整体蛋白质定位(localizome)的解析揭示了意想不到的复杂性,突出了蛋白质多功能性和细胞内定位的重要性。同样,对完整细菌代谢网络的分析也再次显示出高含量的多功能酶以及意想不到的高水平代谢反应和适应性。总而言之,这些新颖的方法已经使最小的细菌之一肺炎支原体的整个生理景观得以破译。在这里,我们总结并讨论了旨在确定任何原核生物蓝图的最新发现。

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