Database of articles cited by EMDB/PDB/SASBDB data

Keywords
Structure methods	All X-ray diffraction NMR electron microscopy small angle scattering neutron diffraction fiber diffraction powder diffraction infrared spectroscopy EPR fluorescence transfer theoretical model Hybrid
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Journal
IF	>30 >20 >10 >5 all

Title	Zinc binding alters the conformational dynamics and drives the transport cycle of the cation diffusion facilitator YiiP.
Journal, issue, pages	J Gen Physiol, Vol. 153, Issue 8, Year 2021
Publish date	Aug 2, 2021
Authors	Maria Lopez-Redondo / Shujie Fan / Akiko Koide / Shohei Koide / Oliver Beckstein / David L Stokes /
PubMed Abstract	YiiP is a secondary transporter that couples Zn2+ transport to the proton motive force. Structural studies of YiiP from prokaryotes and Znt8 from humans have revealed three different Zn2+ sites and a ...YiiP is a secondary transporter that couples Zn2+ transport to the proton motive force. Structural studies of YiiP from prokaryotes and Znt8 from humans have revealed three different Zn2+ sites and a conserved homodimeric architecture. These structures define the inward-facing and outward-facing states that characterize the archetypal alternating access mechanism of transport. To study the effects of Zn2+ binding on the conformational transition, we use cryo-EM together with molecular dynamics simulation to compare structures of YiiP from Shewanella oneidensis in the presence and absence of Zn2+. To enable single-particle cryo-EM, we used a phage-display library to develop a Fab antibody fragment with high affinity for YiiP, thus producing a YiiP/Fab complex. To perform MD simulations, we developed a nonbonded dummy model for Zn2+ and validated its performance with known Zn2+-binding proteins. Using these tools, we find that, in the presence of Zn2+, YiiP adopts an inward-facing conformation consistent with that previously seen in tubular crystals. After removal of Zn2+ with high-affinity chelators, YiiP exhibits enhanced flexibility and adopts a novel conformation that appears to be intermediate between inward-facing and outward-facing states. This conformation involves closure of a hydrophobic gate that has been postulated to control access to the primary transport site. Comparison of several independent cryo-EM maps suggests that the transition from the inward-facing state is controlled by occupancy of a secondary Zn2+ site at the cytoplasmic membrane interface. This work enhances our understanding of individual Zn2+ binding sites and their role in the conformational dynamics that govern the transport cycle.
External links	J Gen Physiol / PubMed:34254979 / PubMed Central
Methods	EM (single particle)
Resolution	3.42 - 4.0 Å
Structure data	23092 7kzx EMDB-23092, PDB-7kzx: Cryo-EM structure of YiiP-Fab complex in Apo state Method: EM (single particle) / Resolution: 4.0 Å 23093 7kzz EMDB-23093, PDB-7kzz: Cryo-EM structure of YiiP-Fab complex in Holo state Method: EM (single particle) / Resolution: 3.42 Å
Chemicals	ChemComp-ZN: Unknown entry
Source	shewanella oneidensis (bacteria) homo sapiens (human)
Keywords	MEMBRANE PROTEIN / Zinc / transporter / cation diffusion facilitator / holo state / inward-facing state / Zinc transport