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
Author
Journal
IF	>30 >20 >10 >5 all

Title	A fiducial-assisted strategy compatible with resolving small MFS transporter structures in multiple conformations using cryo-EM.
Journal, issue, pages	Nat Commun, Vol. 16, Issue 1, Page 7, Year 2025
Publish date	Jan 2, 2025
Authors	Pujun Xie / Yan Li / Gaëlle Lamon / Huihui Kuang / Da-Neng Wang / Nathaniel J Traaseth /
PubMed Abstract	Advancements in cryo-EM have stimulated a revolution in structural biology. Yet, for membrane proteins near the cryo-EM size threshold of approximately 40 kDa, including transporters and G-protein ...Advancements in cryo-EM have stimulated a revolution in structural biology. Yet, for membrane proteins near the cryo-EM size threshold of approximately 40 kDa, including transporters and G-protein coupled receptors, the absence of distinguishable structural features makes image alignment and structure determination a significant challenge. Furthermore, resolving more than one protein conformation within a sample, a major advantage of cryo-EM, represents an even greater degree of difficulty. Here, we describe a strategy for introducing a rigid fiducial marker (BRIL domain) at the C-terminus of membrane transporters from the Major Facilitator Superfamily (MFS) with AlphaFold2. This approach involves fusion of the last transmembrane domain helix of the target protein with the first helix of BRIL through a short poly-alanine linker to promote helicity. Combining this strategy with a BRIL-specific Fab, we elucidated four cryo-EM structures of the 42 kDa Staphylococcus aureus transporter NorA, three of which were derived from a single sample corresponding to inward-open, inward-occluded, and occluded conformations. Hence, this fusion construct facilitated experiments to characterize the conformational landscape of NorA and validated our design to position the BRIL/antibody pair in an orientation that avoids steric clash with the transporter. The latter was enabled through AlphaFold2 predictions, which minimized guesswork and reduced the need for screening several constructs. We further validated the suitability of the method to three additional MFS transporters (GlpT, Bmr, and Blt), results that supported a rigid linker between the transporter and BRIL. The successful application to four MFS proteins, the largest family of secondary transporters in nature, and analysis of predicted structures for the family indicates this strategy will be a valuable tool for studying other MFS members using cryo-EM.
External links	Nat Commun / PubMed:39746942 / PubMed Central
Methods	EM (single particle)
Resolution	2.56 - 3.25 Å
Structure data	44143 9b3k EMDB-44143, PDB-9b3k: NorA in complex with Fab36 (NorA-BRIL fusion) Method: EM (single particle) / Resolution: 2.56 Å 44144 9b3l EMDB-44144, PDB-9b3l: NorA in occluded conformation (NorA-BRIL fusion) Method: EM (single particle) / Resolution: 3.25 Å 44145 9b3m EMDB-44145, PDB-9b3m: NorA in inward-open conformation (NorA-BRIL fusion) Method: EM (single particle) / Resolution: 3.21 Å 44147 9b3o EMDB-44147, PDB-9b3o: NorA in inward-occluded conformation (NorA-BRIL fusion) Method: EM (single particle) / Resolution: 3.18 Å
Source	staphylococcus aureus (bacteria) homo sapiens (human)
Keywords	TRANSPORT PROTEIN/IMMUNE SYSTEM / membrane protein / Staphylococcus aureus / antibiotic resistance / efflux pump / TRANSPORT PROTEIN / TRANSPORT PROTEIN-IMMUNE SYSTEM complex