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	The universal suppressor mutation restores membrane budding defects in the HSV-1 nuclear egress complex by stabilizing the oligomeric lattice.
Journal, issue, pages	PLoS Pathog, Vol. 20, Issue 1, Page e1011936, Year 2024
Publish date	Jan 16, 2024
Authors	Elizabeth B Draganova / Hui Wang / Melanie Wu / Shiqing Liao / Amber Vu / Gonzalo L Gonzalez-Del Pino / Z Hong Zhou / Richard J Roller / Ekaterina E Heldwein /
PubMed Abstract	Nuclear egress is an essential process in herpesvirus replication whereby nascent capsids translocate from the nucleus to the cytoplasm. This initial step of nuclear egress-budding at the inner ...Nuclear egress is an essential process in herpesvirus replication whereby nascent capsids translocate from the nucleus to the cytoplasm. This initial step of nuclear egress-budding at the inner nuclear membrane-is coordinated by the nuclear egress complex (NEC). Composed of the viral proteins UL31 and UL34, NEC deforms the membrane around the capsid as the latter buds into the perinuclear space. NEC oligomerization into a hexagonal membrane-bound lattice is essential for budding because NEC mutants designed to perturb lattice interfaces reduce its budding ability. Previously, we identified an NEC suppressor mutation capable of restoring budding to a mutant with a weakened hexagonal lattice. Using an established in-vitro budding assay and HSV-1 infected cell experiments, we show that the suppressor mutation can restore budding to a broad range of budding-deficient NEC mutants thereby acting as a universal suppressor. Cryogenic electron tomography of the suppressor NEC mutant lattice revealed a hexagonal lattice reminiscent of wild-type NEC lattice instead of an alternative lattice. Further investigation using x-ray crystallography showed that the suppressor mutation promoted the formation of new contacts between the NEC hexamers that, ostensibly, stabilized the hexagonal lattice. This stabilization strategy is powerful enough to override the otherwise deleterious effects of mutations that destabilize the NEC lattice by different mechanisms, resulting in a functional NEC hexagonal lattice and restoration of membrane budding.
External links	PLoS Pathog / PubMed:38227586 / PubMed Central
Methods	EM (subtomogram averaging) / X-ray diffraction
Resolution	3.92 - 13.1 Å
Structure data	EMDB-40223: Cryo-ET reconstruction of WT HSV-1 NEC coat Method: EM (subtomogram averaging) / Resolution: 5.9 Å EMDB-40224: Cryo-ET reconstruction of HSV-1 DN/SUP mutant NEC coat Method: EM (subtomogram averaging) / Resolution: 5.4 Å EMDB-40225: Cryo-ET reconstruction of HSV-1 SUP mutant NEC coat Method: EM (subtomogram averaging) / Resolution: 13.1 Å PDB-8g6d: HSV-1 Nuclear Egress Complex (SUP; UL31-R229L) Method: X-RAY DIFFRACTION / Resolution: 3.92 Å
Chemicals	ChemComp-ZN: Unknown entry ChemComp-HOH: WATER / Water
Source	human alphaherpesvirus 1 strain 17
Keywords	VIRAL PROTEIN / viral nuclear egress complex