Amaya Kensey R, Kocherginskaya Svetlana A, Mackie Roderick I, Cann Isaac K O
Department of Animal Sciences, 1207 W. Gregory Dr., University of Illinois at Urbana-Champaign, Urbana, IL 61801, USA.
J Bacteriol. 2005 Nov;187(21):7481-91. doi: 10.1128/JB.187.21.7481-7491.2005.
Two different genes encoding glutamine synthetase type I (GSI) and GSIII were identified in the genome sequence of R. albus 8. The identity of the GSIII protein was confirmed by the presence of its associated conserved motifs. The glnN gene, encoding the GSIII, was cloned and expressed in Escherichia coli BL21 cells. The recombinant protein was purified and subjected to biochemical and physical analyses. Subunit organization suggested a protein present in solution as both monomers and oligomers. Kinetic studies using the forward and the gamma-glutamyl transferase (gamma-GT) assays were carried out. Mutations that changed conserved glutamic acid residues to alanine in the four GSIII motifs resulted in drastic decreases in GS activity using both assays, except for an E380A mutation, which rather resulted in an increase in activity in the forward assay compared to the wild-type protein. Reduced GSIII activity was also exhibited by mutating, individually, two lysines (K308 and K318) located in the putative nucleotide-binding site to alanine. Most importantly, the presence of mRNA transcripts of the glnN gene in R. albus 8 cells grown under ammonia limiting conditions, whereas little or no transcript was detected in cells grown under ammonia sufficient conditions, suggested an important role for the GSIII in the nitrogen metabolism of R. albus 8. Furthermore, the mutational studies on the conserved GSIII motifs demonstrated, for the first time, their importance in the structure and/or function of a GSIII protein.
在白腐菌8的基因组序列中鉴定出了两种不同的编码I型谷氨酰胺合成酶(GSI)和GSIII的基因。GSIII蛋白的身份通过其相关保守基序的存在得以确认。编码GSIII的glnN基因被克隆并在大肠杆菌BL21细胞中表达。重组蛋白被纯化并进行了生化和物理分析。亚基组成表明该蛋白在溶液中以单体和寡聚体形式存在。使用正向和γ-谷氨酰转移酶(γ-GT)测定法进行了动力学研究。在四个GSIII基序中将保守的谷氨酸残基突变为丙氨酸的突变导致两种测定法中的GS活性急剧下降,但E380A突变除外,与野生型蛋白相比,该突变反而导致正向测定法中的活性增加。将位于假定核苷酸结合位点的两个赖氨酸(K308和K318)分别突变为丙氨酸也表现出GSIII活性降低。最重要的是,在氨限制条件下生长的白腐菌8细胞中存在glnN基因的mRNA转录本,而在氨充足条件下生长的细胞中几乎检测不到或未检测到转录本,这表明GSIII在白腐菌8的氮代谢中起重要作用。此外,对保守的GSIII基序的突变研究首次证明了它们在GSIII蛋白的结构和/或功能中的重要性。