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通过单基因或基因组开放阅读框筛选来选择可溶性/可折叠蛋白质结构域:伯克霍尔德菌假鼻疽抗原BPSL2063头部结构域的结构

Selecting soluble/foldable protein domains through single-gene or genomic ORF filtering: structure of the head domain of Burkholderia pseudomallei antigen BPSL2063.

作者信息

Gourlay Louise J, Peano Clelia, Deantonio Cecilia, Perletti Lucia, Pietrelli Alessandro, Villa Riccardo, Matterazzo Elena, Lassaux Patricia, Santoro Claudio, Puccio Simone, Sblattero Daniele, Bolognesi Martino

机构信息

Department of Biosciences, University of Milan, Via Celoria 26, 20133 Milan, Italy.

Institute of Biomedical Technologies, National Research Council, Via Fratelli Cervi 93, 20090 Segrate, Italy.

出版信息

Acta Crystallogr D Biol Crystallogr. 2015 Nov;71(Pt 11):2227-35. doi: 10.1107/S1399004715015680. Epub 2015 Oct 31.

DOI:10.1107/S1399004715015680
PMID:26527140
Abstract

The 1.8 Å resolution crystal structure of a conserved domain of the potential Burkholderia pseudomallei antigen and trimeric autotransporter BPSL2063 is presented as a structural vaccinology target for melioidosis vaccine development. Since BPSL2063 (1090 amino acids) hosts only one conserved domain, and the expression/purification of the full-length protein proved to be problematic, a domain-filtering library was generated using β-lactamase as a reporter gene to select further BPSL2063 domains. As a result, two domains (D1 and D2) were identified and produced in soluble form in Escherichia coli. Furthermore, as a general tool, a genomic open reading frame-filtering library from the B. pseudomallei genome was also constructed to facilitate the selection of domain boundaries from the entire ORFeome. Such an approach allowed the selection of three potential protein antigens that were also produced in soluble form. The results imply the further development of ORF-filtering methods as a tool in protein-based research to improve the selection and production of soluble proteins or domains for downstream applications such as X-ray crystallography.

摘要

展示了潜在的类鼻疽伯克霍尔德菌抗原和三聚体自转运蛋白BPSL2063保守结构域的1.8 Å分辨率晶体结构,作为类鼻疽病疫苗开发的结构疫苗学靶点。由于BPSL2063(1090个氨基酸)仅含有一个保守结构域,且全长蛋白的表达/纯化存在问题,因此使用β-内酰胺酶作为报告基因构建了一个结构域筛选文库,以进一步筛选BPSL2063的结构域。结果,鉴定出两个结构域(D1和D2),并在大肠杆菌中以可溶形式表达。此外,作为一种通用工具,还构建了来自类鼻疽伯克霍尔德菌基因组的基因组开放阅读框筛选文库,以促进从整个开放阅读框组中选择结构域边界。这种方法筛选出了三种潜在的蛋白质抗原,它们也以可溶形式表达。结果表明,开放阅读框筛选方法可进一步发展成为基于蛋白质研究的一种工具,用于改进可溶性蛋白质或结构域的筛选和生产,以用于如X射线晶体学等下游应用。

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