| Literature DB >> 29588525 |
Biao Qiu1,2, Bingqing Xia3,4, Qingtong Zhou5, Yan Lu1,2, Miaomiao He1,2, Kazuya Hasegawa6, Zhiqiang Ma7, Fengyu Zhang8, Lichuan Gu8, Qionglei Mao3,4, Feng Wang9, Suwen Zhao1,5, Zhaobing Gao10, Jun Liao11,12.
Abstract
Acetate is an important metabolite in metabolism and cell signaling. Succinate-Acetate Permease (SatP) superfamily proteins are known to be responsible for acetate transport across membranes, but the nature of this transport remains unknown. Here, we show that the SatP homolog from Citrobacter koseri (SatP_Ck) is an anion channel that can unidirectionally translocate acetate at rates of the order of ~107 ions/s. Crystal structures of SatP_Ck in complex with multiple acetates at 1.8 Å reveal that the acetate pathway consists of four acetate-binding sites aligned in a single file that are interrupted by three hydrophobic constrictions. The bound acetates at the four sites are each orientated differently. The acetate at the cytoplasmic vestibule is partially dehydrated, whereas those in the main pore body are fully dehydrated. Aromatic residues within the substrate pathway may coordinate translocation of acetates via anion-π interactions. SatP_Ck reveals a new type of selective anion channel and provides a structural and functional template for understanding organic anion transport.Entities:
Mesh:
Substances:
Year: 2018 PMID: 29588525 PMCID: PMC5993801 DOI: 10.1038/s41422-018-0032-8
Source DB: PubMed Journal: Cell Res ISSN: 1001-0602 Impact factor: 25.617