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聚球藻羧基体的分离与特性分析揭示了新型外壳蛋白 CsoS1D 的存在。

Isolation and characterization of the Prochlorococcus carboxysome reveal the presence of the novel shell protein CsoS1D.

机构信息

Department of Chemistry and Biochemistry, The University of Southern Mississippi, Hattiesburg, Mississippi, USA.

出版信息

J Bacteriol. 2012 Feb;194(4):787-95. doi: 10.1128/JB.06444-11. Epub 2011 Dec 9.

Abstract

Cyanobacteria, including members of the genus Prochlorococcus, contain icosahedral protein microcompartments known as carboxysomes that encapsulate multiple copies of the CO(2)-fixing enzyme ribulose 1,5-bisphosphate carboxylase/oxygenase (RubisCO) in a thin protein shell that enhances the catalytic performance of the enzyme in part through the action of a shell-associated carbonic anhydrase. However, the exact mechanism by which compartmentation provides a catalytic advantage to the enzyme is not known. Complicating the study of cyanobacterial carboxysomes has been the inability to obtain homogeneous carboxysome preparations. This study describes the first successful purification and characterization of carboxysomes from the marine cyanobacterium Prochlorococcus marinus MED4. Because the isolated P. marinus MED4 carboxysomes were free from contaminating membrane proteins, their protein complement could be assessed. In addition to the expected shell proteins, the CsoS1D protein that is not encoded by the canonical cso gene clusters of α-cyanobacteria was found to be a low-abundance shell component. This finding and supporting comparative genomic evidence have important implications for carboxysome composition, structure, and function. Our study indicates that carboxysome composition is probably more complex than was previously assumed based on the gene complements of the classical cso gene clusters.

摘要

蓝细菌,包括聚球藻属的成员,含有二十面体蛋白微区室,称为羧基体,它将多个 CO2 固定酶核酮糖 1,5-二磷酸羧化酶/加氧酶(RubisCO)的拷贝包裹在薄的蛋白壳中,通过壳相关碳酸酐酶的作用部分增强酶的催化性能。然而,分隔如何为酶提供催化优势的确切机制尚不清楚。使蓝细菌羧基体的研究复杂化的是无法获得均一的羧基体制剂。本研究描述了从海洋蓝细菌聚球藻 MED4 中首次成功纯化和表征羧基体。由于分离的聚球藻 MED4 羧基体不含污染的膜蛋白,因此可以评估其蛋白质成分。除了预期的壳蛋白外,还发现了一种低丰度的壳蛋白 CsoS1D,它不是α-蓝细菌的典型 cso 基因簇编码的。这一发现和支持的比较基因组证据对羧基体的组成、结构和功能具有重要意义。我们的研究表明,羧基体的组成可能比以前基于经典 cso 基因簇的基因组成所假设的要复杂。

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