Level- Data

Viral proteins

Last updated: 2021 Nov 2

Total hit(s): 5

Select item(s)	Key Findings	Comments (You can add your comments too!)	Original Article (hover to see details)

The kinetics of binding of soluble ACE2 to recombinant RBD was assessed by biolayer interferometry (BLI). The affinity of the B.1.351 RBD to ACE2 was 19-fold higher when compared to the wildtype and 2.7-fold higher when compared to the alpha variant.

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33730597
(Cell)

PMID	33730597 Date of Publishing: 2021 Apr 29
Title	Evidence of escape of SARS-CoV-2 variant B.1.351 from natural and vaccine-induced sera
Author(s) name	Zhou D, Dejnirattisai W et al.
Journal	Cell
Impact factor	27.35 Citation count: 406
Date of Entry	2021 Nov 2

NLM format

Zhou D, Dejnirattisai W, Supasa P, Liu C, Mentzer AJ, Ginn HM, Zhao Y, Duyvesteyn HME, Tuekprakhon A, Nutalai R, Wang B, Paesen GC, Lopez-Camacho C, Slon-Campos J, Hallis B, Coombes N, Bewley K, Charlton S, Walter TS, Skelly D, Lumley SF, Dold C, Levin R, Dong T, Pollard AJ, Knight JC, Crook D, Lambe T, Clutterbuck E, Bibi S, Flaxman A, Bittaye M, Belij-Rammerstorfer S, Gilbert S, James W, Carroll MW, Klenerman P, Barnes E, Dunachie SJ, Fry EE, Mongkolsapaya J, Ren J, Stuart DI, Screaton GR. Evidence of escape of SARS-CoV-2 variant B.1.351 from natural and vaccine-induced sera. Cell. 2021 Apr 29;184(9):2348-2361.e6. PMID:33730597

The D614G spike mutation results in increased viral transduction. However, there was no change in the binding profiles of soluble D614 and G614 spike to human ACE2. The two dissociation constants (KD) were: KD1 = 8.45 nM and KD2 = 127 nM for D614 variant, and KD1 = 18.0 nM and KD2 = 92.7 nM for G614 variant.

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32587969 (33570490)
(bioRxiv)

PMID	32587969 (33570490) Date of Publishing: 2020 Jun 15
Title	The Spike D614G mutation increases SARS-CoV-2 infection of multiple human cell types
Author(s) name	Daniloski Z, Guo X, Sanjana NE.
Journal	bioRxiv
Impact factor	N/A Citation count: 2
Date of Entry	2021 Sep 13

Structure analysis of SARS-CoV-2 N439K Receptor Binding Domain (RBD) in complex with hACE2 at 2.8 resolution showed strong non-covalent salt bridges. These bridges enhanced the binding for hACE2 in the N439K variant, as similar to the SARS-CoV N439R variant. Double mutants of N439K/R and K417V mutations show that salt bridge loss at RBD position 417 is compensated by the one at position 439. This results in hACE2 affinity similar to the wild type.

Methods used for study: X-ray structure, Surface plasmon resonance (SPR) ✍

33621484
(Cell)

PMID	33621484 Date of Publishing: 2021 Jan 28
Title	Circulating SARS-CoV-2 spike N439K variants maintain fitness while evading antibody-mediated immunity
Author(s) name	Thomson EC, Rosen LE et al.
Journal	Cell
Impact factor	27.35 Citation count: 259
Date of Entry	2021 Aug 6

NLM format

Thomson EC, Rosen LE, Shepherd JG, Spreafico R, da Silva Filipe A, Wojcechowskyj JA, Davis C, Piccoli L, Pascall DJ, Dillen J, Lytras S, Czudnochowski N, Shah R, Meury M, Jesudason N, De Marco A, Li K, Bassi J, O'Toole A, Pinto D, Colquhoun RM, Culap K, Jackson B, Zatta F, Rambaut A, Jaconi S, Sreenu VB, Nix J, Zhang I, Jarrett RF, Glass WG, Beltramello M, Nomikou K, Pizzuto M, Tong L, Cameroni E, Croll TI, Johnson N, Di Iulio J, Wickenhagen A, Ceschi A, Harbison AM, Mair D, Ferrari P, Smollett K, Sallusto F, Carmichael S, Garzoni C, Nichols J, Galli M, Hughes J, Riva A, Ho A, Schiuma M, Semple MG, Openshaw PJM, Fadda E, Baillie JK, Chodera JD; ISARIC4C Investigators; COVID-19 Genomics UK (COG-UK) Consortium, Rihn SJ, Lycett SJ, Virgin HW, Telenti A, Corti D, Robertson DL, Snell G. Circulating SARS-CoV-2 spike N439K variants maintain fitness while evading antibody-mediated immunity. Cell. 2021 Mar 4;184(5):1171-1187.e20. PMID:33621484

The binding kinetics of the spike protein of alpha variant and spike of the D614G variant was compared by biolayer interferometry (BLI). A 2-fold decrease was observed in the dissociation constant (Kd) of spike in the alpha variant (Kd=1.3nM) compared to the D614G variant (Kd=3.1nM).

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Pre-print ( bioRXiv )

Title	Impacts on the structure-function relationship of SARS-CoV-2 spike by B.1.1.7 mutations
Impact factor	N/A
Date of Entry	2021 Aug 6

The Y453F and L452R mutations significantly increased the binding affinity to human ACE2 (RBD parental KD = 2.05 0.26 nM; RBD Y453F KD = 0.51 0.06 nM; RBD L452R KD = 1.20 0.06 nM)

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Pre-print ( bioRXiv )

Title	An emerging SARS-CoV-2 mutant evading cellular immunity and increasing viral infectivity
Impact factor	N/A
Date of Entry	2021 Aug 6

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