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肠沙门氏菌 WbaP(UDP-半乳糖:Und-P 半乳糖-1-磷酸转移酶)的 C 末端结构域足以发挥催化活性和特异性,用于结合十一磷酸胞壁酰五肽。

The C-terminal domain of the Salmonella enterica WbaP (UDP-galactose:Und-P galactose-1-phosphate transferase) is sufficient for catalytic activity and specificity for undecaprenyl monophosphate.

机构信息

Department of Microbiology and Immunology, Center for Human Immunology, University of Western Ontario,London, ON, Canada N6A 5C1.

出版信息

Glycobiology. 2012 Jan;22(1):116-22. doi: 10.1093/glycob/cwr114. Epub 2011 Aug 19.

Abstract

Two families of membrane enzymes catalyze the initiation of the synthesis of O-antigen lipopolysaccharide. The Salmonella enterica Typhimurium WbaP is a prototypic member of one of these families. We report here the purification and biochemical characterization of the WbaP C-terminal (WbaP(CT)) domain harboring one putative transmembrane helix and a large cytoplasmic tail. An N-terminal thioredoxin fusion greatly improved solubility and stability of WbaP(CT) allowing us to obtain highly purified protein. We demonstrate that WbaP(CT) is sufficient to catalyze the in vitro transfer of galactose (Gal)-1-phosphate from uridine monophosphate (UDP)-Gal to the lipid carrier undecaprenyl monophosphate (Und-P). We optimized the in vitro assay to determine steady-state kinetic parameters with the substrates UDP-Gal and Und-P. Using various purified polyisoprenyl phosphates of increasing length and variable saturation of the isoprene units, we also demonstrate that the purified enzyme functions highly efficiently with Und-P, suggesting that the WbaP(CT) domain contains all the essential motifs to catalyze the synthesis of the Und-P-P-Gal molecule that primes the biosynthesis of bacterial surface glycans.

摘要

两类膜酶家族催化 O-抗原脂多糖合成的起始。肠沙门氏菌 Typhimurium WbaP 是其中一个家族的典型成员。我们在此报告含有一个假定跨膜螺旋和一个大细胞质尾巴的 WbaP C 末端(WbaP(CT))结构域的纯化和生化特征。N 端硫氧还蛋白融合极大地提高了 WbaP(CT)的可溶性和稳定性,使我们能够获得高度纯化的蛋白质。我们证明 WbaP(CT)足以在体外催化从尿苷二磷酸(UDP)-Gal 到脂质载体十一磷酸(Und-P)的 Gal-1-磷酸的转移。我们优化了体外测定法,以确定与 UDP-Gal 和 Und-P 底物的稳态动力学参数。使用各种长度增加且异戊二烯单位饱和度可变的纯化多异戊二烯磷酸,我们还证明纯化的酶与 Und-P 高度有效地发挥作用,这表明 WbaP(CT)结构域包含所有必需的基序,以催化 Und-P-P-Gal 分子的合成,该分子启动细菌表面聚糖的生物合成。

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