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一种主要易化肽转运蛋白的结构测定:嗜热链球菌内向型肽转运蛋白PepTSt在空间群P3121中结晶。

Structure determination of a major facilitator peptide transporter: Inward facing PepTSt from Streptococcus thermophilus crystallized in space group P3121.

作者信息

Quistgaard Esben M, Martinez Molledo Maria, Löw Christian

机构信息

Centre for Structural Systems Biology (CSSB), DESY and European Molecular Biology Laboratory Hamburg, Hamburg, Germany.

Department of Medical Biochemistry and Biophysics, Karolinska Institutet, Stockholm, Sweden.

出版信息

PLoS One. 2017 Mar 6;12(3):e0173126. doi: 10.1371/journal.pone.0173126. eCollection 2017.

DOI:10.1371/journal.pone.0173126
PMID:28264013
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5338821/
Abstract

Major facilitator superfamily (MFS) peptide transporters (typically referred to as PepT, POT or PTR transporters) mediate the uptake of di- and tripeptides, and so play an important dietary role in many organisms. In recent years, a better understanding of the molecular basis for this process has emerged, which is in large part due to a steep increase in structural information. Yet, the conformational transitions underlying the transport mechanism are still not fully understood, and additional data is therefore needed. Here we report in detail the detergent screening, crystallization, experimental MIRAS phasing, and refinement of the peptide transporter PepTSt from Streptococcus thermophilus. The space group is P3121, and the protein is crystallized in a monomeric inward facing form. The binding site is likely to be somewhat occluded, as the lobe encompassing transmembrane helices 10 and 11 is markedly bent towards the central pore of the protein, but the extent of this potential occlusion could not be determined due to disorder at the apex of the lobe. Based on structural comparisons with the seven previously determined P212121 and C2221 structures of inward facing PepTSt, the structural flexibility as well as the conformational changes mediating transition between the inward open and inward facing occluded states are discussed. In conclusion, this report improves our understanding of the structure and conformational cycle of PepTSt, and can furthermore serve as a case study, which may aid in supporting future structure determinations of additional MFS transporters or other integral membrane proteins.

摘要

主要易化子超家族(MFS)肽转运蛋白(通常称为PepT、POT或PTR转运蛋白)介导二肽和三肽的摄取,因此在许多生物体的饮食中发挥着重要作用。近年来,人们对这一过程的分子基础有了更好的理解,这在很大程度上归功于结构信息的急剧增加。然而,转运机制背后的构象转变仍未完全了解,因此还需要更多数据。在这里,我们详细报告了嗜热链球菌肽转运蛋白PepTSt的去污剂筛选、结晶、实验MIRAS相位测定和精修。空间群为P3121,蛋白质以单体向内的形式结晶。结合位点可能有些封闭,因为包含跨膜螺旋10和11的叶明显向蛋白质的中央孔弯曲,但由于叶顶端的无序,无法确定这种潜在封闭的程度。基于与之前确定的七个向内的PepTSt的P212121和C2221结构的结构比较,讨论了结构灵活性以及介导向内开放和向内封闭状态之间转变的构象变化。总之,本报告增进了我们对PepTSt的结构和构象循环的理解,并且还可以作为一个案例研究,有助于支持未来对其他MFS转运蛋白或其他整合膜蛋白的结构测定。

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