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变异链球菌SMU.2055蛋白晶体结构及其小分子抑制剂设计与筛选
Crystal structure of SMU.2055 protein from Streptococcus mutans and its small molecule inhibitors design and selection

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陈晓丹 1   展秀荣 2   吴昕彧 1   赵春燕 3   赵望泓 1 *  
文摘 目的研究变异链球菌UA159中SMU.2055蛋白的三维晶体结构,并基于其结构进行小分子抑制剂的设计与筛选。方法运用结构基因组学研究方法,通过基因克隆和表达、蛋白质纯化、晶体筛选、晶体衍射数据收集,解析SMU.2055蛋白三维晶体结构,并运用计算机辅助药物设计方法,利用Libdock、Autodock两种程序,通过虚拟筛选和精确对接方式,建立与SMU.2055结构相匹配的小分子抑制剂虚拟模型。结果获得SMU.2055蛋白结晶,解析SMU.2055蛋白三维晶体结构,晶体衍射率为0.23 nm,属于C222_1空间群,晶胞参数为a=9.20 nm,b=9.46 nm,c=19.39 nm,溶剂体积分数为56.7%。设计并筛选出与SMU.2055蛋白结构匹配度高的5个小分子化合物。结论变异链球菌SMU.2055蛋白质晶体学研究有助于从分子水平上深入了解变异链球菌蛋白质的结构和功能,筛选出的5个小分子化合物可能成为SMU.2055的有效小分子抑制剂,所建立的小分子抑制剂虚拟模型为基于蛋白质结构的防龋研究奠定基础。
其他语种文摘 Objective The aim of this study is to analyze the three-dimensional crystal structure of SMU.2055 protein, a putative acetyltransferase from the major caries pathogen Streptococcus mutans (S. mutans). The design and selection of the structure-based small molecule inhibitors are also studied. Methods The three-dimensional crystal structure of SMU.2055 protein was obtained by structural genomics research methods of gene cloning and expression, protein purification with Ni~(2+)- chelating affinity chromatography, crystal screening, and X-ray diffraction data collection. An inhibitor virtual model matching with its target protein structure was set up using computer-aided drug design methods, virtual screening and fine docking, and Libdock and Autodock procedures. Results The crystal of SMU.2055 protein was obtained, and its three-dimensional crystal structure was analyzed. This crystal was diffracted to a resolution of 0.23 nm. It belongs to orthorhombic space group C222_1, with unit cell parameters of a=9.20 nm, b=9.46 nm, and c=19.39 nm. The asymmetric unit contained four molecules, with a solvent content of 56.7%. Moreover, five small molecule compounds, whose structure matched with that of the target protein in high degree, were designed and selected. Conclusion Protein crystallography research of S.mutans SMU.2055 helps to understand the structures and functions of proteins from S.mutans at the atomic level. These five compounds may be considered as effective inhibitors to SMU.2055. The virtual model of small molecule inhibitors we built will lay a foundation to the anticaries research based on the crystal structure of proteins.
来源 华西口腔医学杂志 ,2015,33(2):182-186 【核心库】
DOI 10.7518/hxkq.2015.02.016
关键词 变异链球菌 ; 蛋白质晶体学 ; 小分子抑制剂
地址

1. 南方医科大学南方医院口腔科,南方医科大学口腔医学院, 广州, 510515  

2. 南开大学口腔医院·天津市口腔医院牙体牙髓病科, 天津, 300041  

3. 兰州大学药学院, 兰州, 730000

语种 中文
文献类型 研究性论文
ISSN 1000-1182
学科 生物化学
基金 南方医科大学附属南方医院基金 ;  广东省高校人才引进基金资助项目 ;  国家自然科学基金资助项目
文献收藏号 CSCD:5406218

参考文献 共 8 共1页

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引证文献 2

1 陈璇 变异链球菌UA159中SMU.2055基因在致龋性的作用 南方医科大学学报,2017,37(6):786-791
被引 1

2 李转玲 SMU.2055基因对变异链球菌UA159耐酸能力的影响 南方医科大学学报,2018,38(2):198-204
被引 0 次

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