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Directed assembly of defined oligomeric photosynthetic reaction centres through adaptation with programmable extra-membrane coiled-coil interfaces

机译:通过与可编程的膜外盘绕线圈接口进行适配,可直接组装确定的低聚光合反应中心

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摘要

A challenge associated with the utilisation of bioenergetic proteins in new, synthetic energy transducing systems is achieving efficient and predictable self-assembly of individual components, both natural and man-made, into a functioning macromolecular system. Despite progress with water-soluble proteins, the challenge of programming self-assembly of integral membrane proteins into non-native macromolecular architectures remains largely unexplored. In this work it is shown that the assembly of dimers, trimers or tetramers of the naturally monomeric purple bacterial reaction centre can be directed by augmentation with an α-helical peptide that self-associates into extra-membrane coiled-coil bundle. Despite this induced oligomerisation the assembled reaction centres displayed normal spectroscopic properties, implying preserved structural and functional integrity. Mixing of two reaction centres modified with mutually complementary α-helical peptides enabled the assembly of heterodimers , pointing to a generic strategy for assembling hetero-oligomeric complexes from diverse modified or synthetic components. Addition of two coiled-coil peptides per reaction centre monomer was also tolerated despite the challenge presented to the pigment-protein assembly machinery of introducing multiple self-associating sequences. These findings point to a generalised approach where oligomers or longer range assemblies of multiple light harvesting and/or redox proteins can be constructed in a manner that can be genetically-encoded, enabling the construction of new, designed bioenergetic systems or .
机译:在新的合成能量转换系统中利用生物能蛋白相关的挑战是如何将自然和人造的单个成分高效且可预测地自组装为功能正常的大分子系统。尽管水溶性蛋白取得了进展,但将膜蛋白自组装成非天然大分子结构的程序设计仍面临很大的挑战。在这项工作中表明,天然单体紫色细菌反应中心的二聚体,三聚体或四聚体的组装可以通过自身结合成膜外卷曲螺旋束的α-螺旋肽的引导来进行。尽管发生了这种低聚,组装后的反应中心仍显示出正常的光谱性质,这意味着保留了结构和功能的完整性。两个相互互补的α-螺旋肽修饰的反应中心的混合使异二聚体的组装成为可能,这是从多种修饰或合成组分组装异寡聚复合物的通用策略。尽管对引入多个自缔合序列的色素-蛋白质组装机械提出了挑战,但每个反应中心单体也可容许添加两个卷曲螺旋肽。这些发现指向一种通用的方法,其中可以以可遗传编码的方式构建多个光收集和/或氧化还原蛋白的寡聚物或更长距离的组件,从而能够构建新的,设计的生物能系统。

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