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Crystal Structures of the Serine Protease Domain of Murine Plasma Kallikrein

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【作者】 许明明徐芃周晓雷ANDREASEN Peter江龙光黄明东

【Author】 XU Ming-Ming;XU Peng;ZHOU Xiao-Lei;ANDREASEN Peter;JIANG Long-Guang;HUANG Ming-Dong;University of Chinese Academy of Sciences, State Key Laboratory of Structural Chemistry, Fujian Institute of Research on the Structure of Matter,Chinese Academy of Sciences;Department of Molecular Biology and Genetics, Aarhus University;College of Chemistry, Fuzhou University;

【机构】 University of Chinese Academy of Sciences, State Key Laboratory of Structural Chemistry, Fujian Institute of Research on the Structure of Matter,Chinese Academy of SciencesDepartment of Molecular Biology and Genetics, Aarhus UniversityCollege of Chemistry, Fuzhou University

【摘要】 Plasma kallikrein(PK), a serine protease in the trypsin clan(SA), plays critical roles in many physiological and pathological pathways. Regulating the abnormal activity of PK has been successfully used in the clinical therapy of hereditary angioedema. In this study, the serine protease domain of murine plasma kallikrein(m PK) was expressed in the pichia pastoris system. The recombinant protein was a glycosylated active enzyme after purification by the cation exchange and size-exclusion chromatography, and was crystallized at the precipitant condition of 25% PEG 3350, 0.1 M Tris-HCl pH 8.5 and 0.1 M Na Cl. The crystal structure of m PK was determined at 2.6 ?. This is the first published crystal structure of m PK, showing some distinctive features at S2’ and S3’ pockets when compared to its human analogue(human plasma kallikrein, h PK). In addition, m PK show unique structural features in the non-conservative 67-72 and 76-81 loops when compared to other serine proteases. These results provide insights for the design of potent and selective PK inhibitors.

【Abstract】 Plasma kallikrein(PK), a serine protease in the trypsin clan(SA), plays critical roles in many physiological and pathological pathways. Regulating the abnormal activity of PK has been successfully used in the clinical therapy of hereditary angioedema. In this study, the serine protease domain of murine plasma kallikrein(m PK) was expressed in the pichia pastoris system. The recombinant protein was a glycosylated active enzyme after purification by the cation exchange and size-exclusion chromatography, and was crystallized at the precipitant condition of 25% PEG 3350, 0.1 M Tris-HCl pH 8.5 and 0.1 M Na Cl. The crystal structure of m PK was determined at 2.6 ?. This is the first published crystal structure of m PK, showing some distinctive features at S2’ and S3’ pockets when compared to its human analogue(human plasma kallikrein, h PK). In addition, m PK show unique structural features in the non-conservative 67-72 and 76-81 loops when compared to other serine proteases. These results provide insights for the design of potent and selective PK inhibitors.

【关键词】 murine plasma kallikreinserine proteasespurificationX-ray crystallographyglycosylated
【Key words】 murine plasma kallikreinserine proteasespurificationX-ray crystallographyglycosylated
【基金】 Financially supported by the National Natural Science Foundation of China(31570745,31370737,31400637);the Danish National Research Foundation(26-331-6)
  • 【文献出处】 结构化学 ,Chinese Journal of Structural Chemistry , 编辑部邮箱 ,2017年02期
  • 【分类号】R363
  • 【被引频次】1
  • 【下载频次】55
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