| Literature DB >> 27281193 |
Hirotoshi Tsuchiya1, Shintaro Doki1, Mizuki Takemoto1, Tatsuya Ikuta1, Takashi Higuchi1, Keita Fukui2, Yoshihiro Usuda3, Eri Tabuchi3, Satoru Nagatoishi4, Kouhei Tsumoto4, Tomohiro Nishizawa1, Koichi Ito5, Naoshi Dohmae6, Ryuichiro Ishitani1,7, Osamu Nureki1.
Abstract
The drug/metabolite transporter (DMT) superfamily is a large group of membrane transporters ubiquitously found in eukaryotes, bacteria and archaea, and includes exporters for a remarkably wide range of substrates, such as toxic compounds and metabolites. YddG is a bacterial DMT protein that expels aromatic amino acids and exogenous toxic compounds, thereby contributing to cellular homeostasis. Here we present structural and functional analyses of YddG. Using liposome-based analyses, we show that Escherichia coli and Starkeya novella YddG export various amino acids. The crystal structure of S. novella YddG at 2.4 Å resolution reveals a new membrane transporter topology, with ten transmembrane segments in an outward-facing state. The overall structure is basket-shaped, with a large substrate-binding cavity at the centre of the molecule, and is composed of inverted structural repeats related by two-fold pseudo-symmetry. On the basis of this intramolecular symmetry, we propose a structural model for the inward-facing state and a mechanism of the conformational change for substrate transport, which we confirmed by biochemical analyses. These findings provide a structural basis for the mechanism of transport of DMT superfamily proteins.Entities:
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Year: 2016 PMID: 27281193 DOI: 10.1038/nature17991
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962