组装最小的分裂体。

Systems and Synthetic Biology Pub Date : 2014-09-01 Epub Date: 2014-04-27 DOI:10.1007/s11693-014-9150-x
Zohreh Nourian, Andrew Scott, Christophe Danelon
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摘要

构建具有生命系统所有基本属性的不可还原的最小细胞是合成生物学面临的最大挑战之一。任何生命系统都要完成的一项无处不在的任务就是细胞包膜的分裂。因此,组装一个支持分室分裂的基本(尽管足够)分子机制,是实现自我复制人工细胞的关键一步。向后看可能的祖先细胞分裂系统的分子性质,也就是所谓的更原始的细胞分裂系统,可能有助于确定最小的分裂体。鉴于从简单的脂质囊泡到现代生命的分裂机制的可能进化途径,我们定义了两种重现原始细胞分裂的方法:膜变形蛋白途径和脂质生物合成途径。在确定了参与膜形状改变的可能蛋白质和工作机制后,我们接着讨论了如何将它们整合到依靠脂质体内基因表达的可编程最小细胞的构建框架中。使用重组元件的蛋白质合成(PURE)系统是一种重组的最小基因表达系统,可以说是最通用的合成平台。作为从头合成 divisome 的第一步,我们展示了从其基因中产生的 N-BAR 结构域蛋白可以组装到脂质体的外表面,并将膜雕刻成管状结构。最后,我们讨论了建立自我复制最小细胞的其余挑战,特别是分裂机制与体积扩展和基因组复制的耦合。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Toward the assembly of a minimal divisome.

The construction of an irreducible minimal cell having all essential attributes of a living system is one of the biggest challenges facing synthetic biology. One ubiquitous task accomplished by any living systems is the division of the cell envelope. Hence, the assembly of an elementary, albeit sufficient, molecular machinery that supports compartment division, is a crucial step towards the realization of self-reproducing artificial cells. Looking backward to the molecular nature of possible ancestral, supposedly more rudimentary, cell division systems may help to identify a minimal divisome. In light of a possible evolutionary pathway of division mechanisms from simple lipid vesicles toward modern life, we define two approaches for recapitulating division in primitive cells: the membrane deforming protein route and the lipid biosynthesis route. Having identified possible proteins and working mechanisms participating in membrane shape alteration, we then discuss how they could be integrated into the construction framework of a programmable minimal cell relying on gene expression inside liposomes. The protein synthesis using recombinant elements (PURE) system, a reconstituted minimal gene expression system, is conceivably the most versatile synthesis platform. As a first step towards the de novo synthesis of a divisome, we showed that the N-BAR domain protein produced from its gene could assemble onto the outer surface of liposomes and sculpt the membrane into tubular structures. We finally discuss the remaining challenges for building up a self-reproducing minimal cell, in particular the coupling of the division machinery with volume expansion and genome replication.

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