Di Guilmi A M, Mouz N, Andrieu J P, Hoskins J, Jaskunas S R, Gagnon J, Dideberg O, Vernet T
Institut de Biologie Structurale Jean-Pierre Ebel (CEA/CNRS), 38027 Grenoble Cedex 1, France.
J Bacteriol. 1998 Nov;180(21):5652-9. doi: 10.1128/JB.180.21.5652-5659.1998.
Resistance to beta-lactam antibiotics in Streptococcus pneumoniae is due to alteration of penicillin-binding proteins (PBPs). S. pneumoniae PBP 1a belongs to the class A high-molecular-mass PBPs, which harbor transpeptidase (TP) and glycosyltransferase (GT) activities. The GT active site represents a new potential target for the generation of novel nonpenicillin antibiotics. The 683-amino-acid extracellular region of PBP 1a (PBP 1a*) was expressed in Escherichia coli as a GST fusion protein. The GST-PBP 1a* soluble protein was purified, and its domain organization was revealed by limited proteolysis. A protease-resistant fragment spanning Ser 264 to Arg 653 exhibited a reactivity profile against both beta-lactams and substrate analogues similar to that of the parent protein. This protein fragment represents the TP domain. The GT domain (Ser 37 to Lys 263) was expressed as a recombinant GST fusion protein. Protection by moenomycin of the GT domain against trypsin degradation was interpreted as an interaction between the GT domain and the moenomycin.
肺炎链球菌对β-内酰胺类抗生素的耐药性是由于青霉素结合蛋白(PBPs)的改变。肺炎链球菌PBP 1a属于A类高分子量PBPs,具有转肽酶(TP)和糖基转移酶(GT)活性。GT活性位点是生成新型非青霉素类抗生素的一个新的潜在靶点。PBP 1a的683个氨基酸的细胞外区域(PBP 1a*)在大肠杆菌中作为GST融合蛋白表达。纯化了GST-PBP 1a*可溶性蛋白,并通过有限蛋白酶解揭示了其结构域组织。一个跨越Ser 264至Arg 653的抗蛋白酶片段对β-内酰胺类药物和底物类似物的反应性谱与亲本蛋白相似。该蛋白片段代表TP结构域。GT结构域(Ser 37至Lys 263)作为重组GST融合蛋白表达。莫能菌素对GT结构域的胰蛋白酶降解保护作用被解释为GT结构域与莫能菌素之间的相互作用。