Research Institute of Molecular Pathology, Dr. Bohr-gasse 7, 1030 Vienna, Austria.
J Biol Chem. 2011 Jul 1;286(26):23121-31. doi: 10.1074/jbc.M111.239657. Epub 2011 May 10.
The peptide transporter (PTR) family represents a group of proton-coupled secondary transporters responsible for bulk uptake of amino acids in the form of di- and tripeptides, an essential process employed across species ranging from bacteria to humans. To identify amino acids critical for peptide transport in a prokaryotic PTR member, we have screened a library of mutants of the Escherichia coli peptide transporter YdgR using a high-throughput substrate uptake assay. We have identified 35 single point mutations that result in a full or partial loss of transport activity. Additional analysis, including homology modeling based on the crystal structure of the Shewanella oneidensis peptide transporter PepT(so), identifies Glu(56) and Arg(305) as potential periplasmic gating residues. In addition to providing new insights into transport by members of the PTR family, these mutants provide valuable tools for further study of the mechanism of peptide transport.
肽转运蛋白(PTR)家族代表了一组质子偶联的二级转运蛋白,负责以二肽和三肽的形式摄取大量氨基酸,这是从细菌到人类等各种物种中采用的基本过程。为了确定原核 PTR 成员中对肽转运至关重要的氨基酸,我们使用高通量底物摄取测定法筛选了大肠杆菌肽转运蛋白 YdgR 的突变文库。我们已经鉴定出 35 个单点突变,这些突变导致完全或部分丧失转运活性。进一步的分析,包括基于 Shewanella oneidensis 肽转运蛋白 PepT(so)的晶体结构的同源建模,确定 Glu(56)和 Arg(305)为潜在的周质门控残基。这些突变体除了为 PTR 家族成员的转运提供新的见解外,还为进一步研究肽转运机制提供了有价值的工具。
