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Structure
Last updated: 2022 Jul 13
Total hit(s): 101
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Original Article
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The crystal structure of T6 Fab bound to the RBD of
B.1.351
with three signature mutations K417N/E484K/N501Y (RBD-3M) at 2.89 A resolution, shows that the mutated residues residues N417, K484, and Y501, are not located within the
epitope
of the T6 Fab. L452R
mutation
which is found in several SARS-CoV-2 variants, is not evident in the T6
epitope.
Examination of the enhancement patterns across the single and triple mutant pseudoviruses showed that the 242244del in NTD, K417N/T, and 417N/484K/501Y in RBD were all potential contributors as mAb T6 was able to exert at least a 3-fold increase in neutralization to 3 of the 4 variants of concern, thus suggesting that its epitope might have become more exposed in some of these variants.
✍
35291264
(
iScience
)
PMID
35291264
Date of Publishing
: 2022 Apr 15
Title
RBD trimer mRNA vaccine elicits broad and protective immune responses against SARS-CoV-2 variants
Author(s) name
Liang Q, Wang Y et al.
Journal
iScience
Impact factor
4.447
Citation count
: 1
Date of Entry
2022 Jul 13
×
NLM format
Liang Q, Wang Y, Zhang S, Sun J, Sun W, Li J, Liu Y, Li M, Cheng L, Jiang Y, Wang R, Zhang R, Yang Z, Ren Y, Chen P, Gao P, Yan H, Zhang Z, Zhang Q, Shi X, Wang J, Liu W, Wang X, Ying B, Zhao J, Qi H, Zhang L RBD trimer mRNA vaccine elicits broad and protective immune responses against SARS-CoV-2 variants. iScience. 2022 Apr 15;25(4):104043. PMID:35291264
Cryo-EM structure of monoclonal
antibody
- T6's Fab in complex with
B.1.351
spike trimer protein shows that T6
antibody
binds only to the "up" RBD, therefore the T6
epitope
is buried when the RBD is in the "down" conformation in the spike trimer.
Analysis of T6 epitope residues in the GISAID database revealed a high degree of conservation, thus providing a sequence and structural basis for its broad and potent neutralizing activity against a wide range of SARS-CoV-2 variants.
✍
35291264
(
iScience
)
PMID
35291264
Date of Publishing
: 2022 Apr 15
Title
RBD trimer mRNA vaccine elicits broad and protective immune responses against SARS-CoV-2 variants
Author(s) name
Liang Q, Wang Y et al.
Journal
iScience
Impact factor
4.447
Citation count
: 1
Date of Entry
2022 Jul 13
×
NLM format
Liang Q, Wang Y, Zhang S, Sun J, Sun W, Li J, Liu Y, Li M, Cheng L, Jiang Y, Wang R, Zhang R, Yang Z, Ren Y, Chen P, Gao P, Yan H, Zhang Z, Zhang Q, Shi X, Wang J, Liu W, Wang X, Ying B, Zhao J, Qi H, Zhang L RBD trimer mRNA vaccine elicits broad and protective immune responses against SARS-CoV-2 variants. iScience. 2022 Apr 15;25(4):104043. PMID:35291264
The crystal structure of 3CLpro in complex with Oridonin at a resolution of 2.10 Å shows catalytic residues His41 and Cys145 of 3CLpro
interacting
with Oridonin. Oridonin inhibits SARSCoV2 3CLpro by forming a covalent bond with the sulfhydryl group of Cys145.
Because of Oridonin's nonpeptidomimetic covalent binding mode, it is a novel candidate to develop a new antiviral treatment for COVID-19.
✍
35600064
(
)
PMID
35600064
Title
Oridonin Inhibits SARS-CoV-2 by Targeting Its 3C-Like Protease
Impact factor
N/A
Date of Entry
2022 Jul 13
×
NLM format
Oridonin Inhibits SARS-CoV-2 by Targeting Its 3C-Like Protease. . . PMID:35600064
Structural superimposition of the RBD region of Spike glycoprotein of SARS-CoV-2 wild and its variants -
Omicron,
Delta
AY.1 & 2 and AY. 3, showed structural changes around the
antibody
binding regions. Protein structure prediction showed Omicron's polarity, non-polarity, and hydrophobicity characteristics changed from the wild SARS-CoV-2.
Omicron and Delta AY.3 are expected to be more pathogenic due to their RBD structures' greater instability.
✍
35690234
(
Microb Pathog
)
PMID
35690234
Date of Publishing
: 2022 Jun 8
Title
The influence of new SARS-CoV-2 variant Omicron (B.1.1.529) on vaccine efficacy, its correlation to Delta variants: A computational approach
Author(s) name
Ranjan P, Neha et al.
Journal
Microb Pathog
Impact factor
2.64
Citation count
: 1
Date of Entry
2022 Jun 27
×
NLM format
Ranjan P, Neha, Devi C, Devar KA, Das P The influence of new SARS-CoV-2 variant Omicron (B.1.1.529) on vaccine efficacy, its correlation to Delta variants: A computational approach. Microb Pathog. 2022 Jun 8;169:105619. PMID:35690234
X-ray diffraction structures of Nirmatrelvir (PF-07321332) with M
pro
of variants of concern having mutations
[Alpha,
Beta,
Gamma(
K90R),
Lambda
(G15S) and
Omicron
(P132H)], show that the
binding
of nirmatrelvir is not disturbed by the mutations. The ligand has the same protein
interactions
as observed in the wild type M
Pro
from the variant
USA-
WA1/2020.
1. The crystal structures also show that the mutations do not give rise to any signification changes of the protein around the binding pocket or the site of the mutation.
2. The catalytic efficiencies (kcat/Km) of the K90R (28255 S
-1
M
-1
), G15S (16483 S
-1
M
-1
), and P132H (22692 S
-1
M
-1
) are similar to wildtype M
pro
(39830 S
-1
M
-1
).
3. Nirmatrelvir potently inhibited wildtype (mean Ki of 0.93 nM) and the mutated enzymes containing the K90R (Ki 1.05nM), G15S (Ki 4.07 nM) and P132H (Ki 0.64 nM)M
pro
.
✍
~
(
)
PMID
~
Title
Structural basis for Nirmatrelvir in vitro efficacy against SARS-CoV-2 variants
Impact factor
N/A
Date of Entry
2022 Mar 11
×
NLM format
Structural basis for Nirmatrelvir in vitro efficacy against SARS-CoV-2 variants. . . PMID:~
Cryo-EM structure of the
Omicron
variant
spike protein
in complex with human
ACE2
reveals salt bridge between RBD N417 and
ACE2
D30 is lost. R493, R498 form salt bridge with
ACE2
residues E35, D38, respectively and S496 forms a hydrogen bond with
ACE2
residue K353.
Compared to the Delta variant, new interactions are formed as a result of the mutations Q493R, G496S and Q498R, and the salt bridge between RBD K417 and ACE2 D30 is lost.
✍
Pre-print
(
bioRXiv
)
Title
SARS-CoV-2 Omicron Variant: ACE2 Binding, Cryo-EM Structure of Spike Protein-ACE2 Complex and Antibody Evasion
Impact factor
N/A
Date of Entry
2022 Jan 10
The trimer organisation of the Omicron
spike protein
ectodomain is similar to that of the original strain and all the earlier variants, according to cryo-EM structural study. The
Omicron
variant has 37 mutations in the
spike protein,
and 15 of which are in the receptor
binding
region (RBD)
The Omicron variant spike protein contains 3-5 times the number of mutations found in prior SARS-CoV-2 strains. Understanding the effects of these mutations on ACE2 receptor binding and neutralising antibody evasion is critical for developing effective therapies to stop the spread of the Omicron and related variations.
✍
Pre-print
(
bioRXiv
)
Title
SARS-CoV-2 Omicron Variant: ACE2 Binding, Cryo-EM Structure of Spike Protein-ACE2 Complex and Antibody Evasion
Impact factor
N/A
Date of Entry
2022 Jan 10
Structural analysis was done to show the position of mutated residues in the
Lambda
spike regions (NTD and RBD). Three mutations (G75V, T76I, and RSYLTPGD246-253N) were presentin theN-terminal domain (NTD)and the
deletion
mutation (RSYLTPGD246-253N
)mutation
was observedin a loop structure(loop 5).Another protein region (Receptor
binding
domain) containstwo mutations (L452Q and F490S). In addition, the T859N
mutation
wasfound in a specificSpikesubunit (S2heptad repeat 1).
Loop 5 contains 246-260 residues, which was a loop structure designated in a previous study.
✍
Pre-print
(
bioRXiv
)
Title
SARS-CoV-2 Lambda variant exhibits higher infectivity and immune resistance
Impact factor
N/A
Date of Entry
2021 Dec 15
A unique drug targeting pocket of 279 ų volume is predicted on the SARS-CoV-2
N-
NTD. It has a druggability score between 0 and 1.
SARS-CoV N-NTD and MERS-CoV N-NTD pocket volumes similar to SARS-CoV-2N-NTD but HCoV-OC43 has a larger pocket with a volume of 352 3Å ³.
✍
32363136
(
Acta Pharm Sin B
)
PMID
32363136
Date of Publishing
: 2020 Jul
Title
Crystal structure of SARS-CoV-2 nucleocapsid protein RNA binding domain reveals potential unique drug targeting sites
Author(s) name
Kang S, Yang M et al.
Journal
Acta Pharm Sin B
Impact factor
6.15
Citation count
: 271
Date of Entry
2021 Nov 8
×
NLM format
Kang S, Yang M, Hong Z, Zhang L, Huang Z, Chen X, He S, Zhou Z, Zhou Z, Chen Q, Yan Y, Zhang C, Shan H, Chen S. Crystal structure of SARS-CoV-2 nucleocapsid protein RNA binding domain reveals potential unique drug targeting sites. Acta Pharm Sin B. 2020 Jul;10(7):1228-1238. PMID:32363136
Structure of SARS-CoV-2 nsp16/nsp10 in complex with
RNA
cap analogue (m7GpppA) and
S-
adenosylmethionine (SAM), which methylates 2-OH of ribose of the first transcribing nucleotide of the mRNA cap. It causes conformational changes in
nsp16
and an alternate ligand
binding
site in
nsp16
which can be a target for antiviral development.
The structure also reveals the basis of an induced fit model of the RNA cap binding and 2-O methylation of the first transcribing nucleotide of SARS-CoV-2 genome.
✍
32709886
(
Nat Commun
)
PMID
32709886
Date of Publishing
: 2020 Jul 24
Title
Structural basis of RNA cap modification by SARS-CoV-2
Author(s) name
Viswanathan T, Arya S et al.
Journal
Nat Commun
Impact factor
11.8
Citation count
: 92
Date of Entry
2021 Oct 27
×
NLM format
Viswanathan T, Arya S, Chan SH, Qi S, Dai N, Misra A, Park JG, Oladunni F, Kovalskyy D, Hromas RA, Martinez-Sobrido L, Gupta YK. Structural basis of RNA cap modification by SARS-CoV-2. Nat Commun. 2020 Jul 24;11(1):3718. PMID:32709886
The conformational changes of the
spike protein
was studied along with the effect of D614G
mutation
on the soluble
S
ectodomain construct. The G614 variant exhibited enhanced furin cleavage efficiency and modified RBD constitution.
The study used engineered soluble construct. The similarity of these to the native virion context should be studied further. Also, the effect of the D614G mutation on cleavage at the TMPRSS2 cleavage site should be studied.
✍
33417835
(
Cell Rep
)
PMID
33417835
Date of Publishing
: 2021 Jan 12
Title
D614G Mutation Alters SARS-CoV-2 Spike Conformation and Enhances Protease Cleavage at the S1/S2 Junction
Author(s) name
Gobeil SM, Janowska K et al.
Journal
Cell Rep
Impact factor
7.7
Citation count
: 98
Date of Entry
2021 Oct 27
×
NLM format
Gobeil SM, Janowska K, McDowell S, Mansouri K, Parks R, Manne K, Stalls V, Kopp MF, Henderson R, Edwards RJ, Haynes BF, Acharya P. D614G Mutation Alters SARS-CoV-2 Spike Conformation and Enhances Protease Cleavage at the S1/S2 Junction. Cell Rep. 2021 Jan 12;34(2):108630. PMID:33417835
The crystal structure of SARS-CoV2 CTD reveals its role in viral RNA
binding
and its interaction with transcriptional regulatory sequences. 5 unpaired adeno dinucleotide in the stem-loop region of TRS-L is a key factor involved in the
binding
of nucleocapsid protein
It is reported that in SARS-CoV, the N-NTD, N-CTD, and C-IDR domains are to bind the viral RNA. Even so, the roles of them in RNA binding is yet to be determined.
✍
33511102
(
Front Chem
)
PMID
33511102
Date of Publishing
: 2020
Title
Structural Insight Into the SARS-CoV-2 Nucleocapsid Protein C-Terminal Domain Reveals a Novel Recognition Mechanism for Viral Transcriptional Regulatory Sequences
Author(s) name
Yang M, He S et al.
Journal
Front Chem
Impact factor
3.42
Citation count
: 20
Date of Entry
2021 Oct 27
×
NLM format
Yang M, He S, Chen X, Huang Z, Zhou Z, Zhou Z, Chen Q, Chen S, Kang S. Structural Insight Into the SARS-CoV-2 Nucleocapsid Protein C-Terminal Domain Reveals a Novel Recognition Mechanism for Viral Transcriptional Regulatory Sequences. Front Chem. 2021 Jan 12;8:624765. PMID:33511102
The cryo-EM structure of the
S
protein of the
Alpha
variant in the apo form and receptor ACE-2 bound form were charecterised. The A570D
mutation
modulates the opening and closing of the receptor
binding
domain (RBD) by introducing a salt bridge. The N501Y
mutation
increases ACE-2
binding
affinity by introducing pi-pi interaction.
✍
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 Sep 13
Structure of SARS-CoV-2
ORF8
accessory protein reveals a 60-residue core.It has is 16% sequence identity to SARS-CoV-2
ORF7a,
a covalent disulfide linked dimer and a non-covalent dimer formed by 73YIDI76 sequence.
ORF8 antibodies are major serological markers of SARS-CoV-2 infection.
✍
33361333
(
Proc Natl Acad Sci U S A
)
PMID
33361333
Date of Publishing
: 2021 Jan 12
Title
Structure of SARS-CoV-2 ORF8, a rapidly evolving coronavirus protein implicated in immune evasion
Author(s) name
Flower TG, Buffalo CZ et al.
Journal
Proc Natl Acad Sci U S A
Impact factor
9.35
Citation count
: 84
Date of Entry
2021 Aug 22
×
NLM format
Flower TG, Buffalo CZ, Hooy RM, Allaire M, Ren X, Hurley JH. Structure of SARS-CoV-2 ORF8, a rapidly evolving coronavirus protein implicated in immune evasion. Proc Natl Acad Sci U S A. 2021 Jan 12;118(2):e2021785118. PMID:33361333
Neuropilin-1 b1 domain binds with SARS-CoV-2 S1 C-end rule (CendR) peptide (7 residues -679-NSPRRAR-685) with an affinity of 20.3 µM at pH 7.5, and 13.0 µM at pH 5.5. In NRP1-depleted Caco-2 cells, viral uptake is halved compared to control cells.
Blocking the interaction of NRP1-b1 with SARS-CoV-2 S1 CendR with inhibitors like EG00229 can lead to new anti COVID-19 therapeutics.
✍
33082294
(
Science
)
PMID
33082294
Date of Publishing
: 2020 Nov 13
Title
Neuropilin-1 is a host factor for SARS-CoV-2 infection
Author(s) name
Daly JL, Simonetti B et al.
Journal
Science
Impact factor
20.57
Citation count
: 477
Date of Entry
2021 Aug 2
×
NLM format
Daly JL, Simonetti B, Klein K, Chen KE, Williamson MK, Antón-Plágaro C, Shoemark DK, Simón-Gracia L, Bauer M, Hollandi R, Greber UF, Horvath P, Sessions RB, Helenius A, Hiscox JA, Teesalu T, Matthews DA, Davidson AD, Collins BM, Cullen PJ, Yamauchi Y. Neuropilin-1 is a host factor for SARS-CoV-2 infection. Science. 2020 Nov 13;370(6518):861-865. PMID:33082294
Structure of SARS-CoV-2
Nsp15
endoribonuclease with Uridine-2',3'-Vanadate (UV, a transition state analog), results in the formation of 2′,3′-cyclic phosphodiester. This is critical for further
RNA
maturation and functions.
This structure proposes that Nsp15 should follow a two-step reaction mechanism with the final product being 3UMP.
✍
33564093
(
Commun Biol
)
PMID
33564093
Date of Publishing
: 2021 Feb 9
Title
Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2
Author(s) name
Kim Y, Wower J et al.
Journal
Commun Biol
Impact factor
N/A
Citation count
: 34
Date of Entry
2021 Aug 2
×
NLM format
Kim Y, Wower J, Maltseva N, Chang C, Jedrzejczak R, Wilamowski M, Kang S, Nicolaescu V, Randall G, Michalska K, Joachimiak A. Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2. Commun Biol. 2021 Feb 9;4(1):193. PMID:33564093
The structure of Tipiracil (a uracil derivative ) and SARS-CoV-2
Nsp15
endoribonuclease shows Tipiracil competitively inhibits the enzyme action by
binding
to its active site.
Structure illustrates that uracil alone probably has similar inhibitory properties and provides basis for the uracil scaffold-based drug development.
✍
33564093
(
Commun Biol
)
PMID
33564093
Date of Publishing
: 2021 Feb 9
Title
Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2
Author(s) name
Kim Y, Wower J et al.
Journal
Commun Biol
Impact factor
N/A
Citation count
: 34
Date of Entry
2021 Aug 2
×
NLM format
Kim Y, Wower J, Maltseva N, Chang C, Jedrzejczak R, Wilamowski M, Kang S, Nicolaescu V, Randall G, Michalska K, Joachimiak A. Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2. Commun Biol. 2021 Feb 9;4(1):193. PMID:33564093
Structure of SARS-CoV-2
Nsp15
endoribonuclease in complex with dinucleoside monophosphate (GpU), which binds to the active site of the enzyme with uracil
interacting
with Tyr343 and Ser294. This results in the SARS-CoV-2
Nsp15
is
inhibition.
Complex structure demonstrates location and specificity determinants of the uridine with a 5-phosphoryl group. Nsp15 is shown to bind and hydrolyze 4, 7, and 20 nucleotide long RNA. Comparitive study of Nsp15 and RNase A active site displayed some conserved active site residues and indicated a common catalytic mechanism with a two-step reaction releasing 3UMP, despite distinct RNA binding site organization in both including both sequence and structure dissimilarity.
✍
33564093
(
Commun Biol
)
PMID
33564093
Date of Publishing
: 2021 Feb 9
Title
Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2
Author(s) name
Kim Y, Wower J et al.
Journal
Commun Biol
Impact factor
N/A
Citation count
: 34
Date of Entry
2021 Aug 2
×
NLM format
Kim Y, Wower J, Maltseva N, Chang C, Jedrzejczak R, Wilamowski M, Kang S, Nicolaescu V, Randall G, Michalska K, Joachimiak A. Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2. Commun Biol. 2021 Feb 9;4(1):193. PMID:33564093
Structure of SARS-CoV-2
Nsp15
endoribonuclease in complex with 3'-uridine monophosphate shows uracil demonstrates higher affinity for Trp333 site than in uracil-recognition site created by His235, His250, and Thr341.
Structure emphasis that since the enzyme's substrate is a larger RNA molecule, the identity of the Trp333-interacting base is inappropriate.
✍
33564093
(
Commun Biol
)
PMID
33564093
Date of Publishing
: 2021 Feb 9
Title
Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2
Author(s) name
Kim Y, Wower J et al.
Journal
Commun Biol
Impact factor
N/A
Citation count
: 34
Date of Entry
2021 Aug 2
×
NLM format
Kim Y, Wower J, Maltseva N, Chang C, Jedrzejczak R, Wilamowski M, Kang S, Nicolaescu V, Randall G, Michalska K, Joachimiak A. Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2. Commun Biol. 2021 Feb 9;4(1):193. PMID:33564093
SARS-CoV-2
Nsp15
is inhibited by
interactions
with the uridine
binding
pocket in the enzyme's active site. Structure of SARS CoV-2
Nsp15
endoribonuclease in complex with Uridine-5'-Monophosphate shows
Nsp15
discriminates between the uracil and purine bases by forming van der Waals contacts with Tyr343 and hydrogen bonds Ser294 (an active site residue ).
Nsp15 enzyme is inhibited by the binding of 5'-UMP in the uracil binding pocket.
✍
33564093
(
Commun Biol
)
PMID
33564093
Date of Publishing
: 2021 Feb 9
Title
Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2
Author(s) name
Kim Y, Wower J et al.
Journal
Commun Biol
Impact factor
N/A
Citation count
: 34
Date of Entry
2021 Aug 2
×
NLM format
Kim Y, Wower J, Maltseva N, Chang C, Jedrzejczak R, Wilamowski M, Kang S, Nicolaescu V, Randall G, Michalska K, Joachimiak A. Tipiracil binds to uridine site and inhibits Nsp15 endoribonuclease NendoU from SARS-CoV-2. Commun Biol. 2021 Feb 9;4(1):193. PMID:33564093
The pseudoknot at the entry to the mRNA channel is a key structural characteristic for translation of the SARS-CoV-2
RNA
genome. It specifically interacts with ribosomal proteins (Rabbit 80S ribosome) and 18S rRNA and causes ribosomal pausing prior to -1 frameshifting and the translating ribosome structure. Here, rabbit 80S ribosome colliding in another ribosome stalled by the SARS-CoV-2 pseudoknot is structurally characterized.
Interfering with the frameshifting process at the level of nascent chain interactions with the ribosomal tunnel at the level of RNA folding leads to the formation of the frameshift stimulatory pseudoknot, representing a viable strategy in the search for new drugs against SARS-CoV-2.
✍
34029205
(
Science
)
PMID
34029205
Date of Publishing
: 2021 Jun 18
Title
Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome
Author(s) name
Bhatt PR, Scaiola A et al.
Journal
Science
Impact factor
20.57
Citation count
: 51
Date of Entry
2021 Aug 11
×
NLM format
Bhatt PR, Scaiola A, Loughran G, Leibundgut M, Kratzel A, Meurs R, Dreos R, O'Connor KM, McMillan A, Bode JW, Thiel V, Gatfield D, Atkins JF, Ban N. Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome. Science. 2021 Jun 18;372(6548):1306-1313. PMID:34029205
The pseudoknot at the entry to the mRNA channel is a key structural characteristic for translation of the SARS-CoV-2
RNA
genome. It specifically interacts with ribosomal proteins (Rabbit 80S ribosome) and 18S rRNA and causes ribosomal pausing prior to -1 frameshifting and the translating ribosome structure. By cryo-electron microscopy the structure of rabbit 80S ribosome in complex with eRF1 and ABCE1, stalled at the STOP codon in the mutated SARS-CoV-2 slippery site is studied.
Interfering with the frameshifting process at the level of nascent chain interactions with the ribosomal tunnel at the level of RNA folding leads to the formation of the frameshift stimulatory pseudoknot, representing a viable strategy in the search for new drugs against SARS-CoV-2.
✍
34029205
(
Science
)
PMID
34029205
Date of Publishing
: 2021 Jun 18
Title
Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome
Author(s) name
Bhatt PR, Scaiola A et al.
Journal
Science
Impact factor
20.57
Citation count
: 51
Date of Entry
2021 Aug 11
×
NLM format
Bhatt PR, Scaiola A, Loughran G, Leibundgut M, Kratzel A, Meurs R, Dreos R, O'Connor KM, McMillan A, Bode JW, Thiel V, Gatfield D, Atkins JF, Ban N. Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome. Science. 2021 Jun 18;372(6548):1306-1313. PMID:34029205
The pseudoknot at the entry to the mRNA channel is a key structural characteristic for translation of the SARS-CoV-2
RNA
genome. It specifically interacts with ribosomal proteins (Rabbit 80S ribosome) and 18S rRNA and causes ribosomal pausing prior to -1 frameshifting and the translating ribosome structure was studied by cryo-electron microscopy. The rabbit 80S ribosome is stalled close to the mutated SARS-CoV-2 slippery site by a pseudoknot.
Interfering with the frameshifting process at the level of nascent chain interactions with the ribosomal tunnel at the level of RNA folding leads to the formation of the frameshift stimulatory pseudoknot, representing a viable strategy in the search for new drugs against SARS-CoV-2.
✍
34029205
(
Science
)
PMID
34029205
Date of Publishing
: 2021 Jun 18
Title
Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome
Author(s) name
Bhatt PR, Scaiola A et al.
Journal
Science
Impact factor
20.57
Citation count
: 51
Date of Entry
2021 Aug 11
×
NLM format
Bhatt PR, Scaiola A, Loughran G, Leibundgut M, Kratzel A, Meurs R, Dreos R, O'Connor KM, McMillan A, Bode JW, Thiel V, Gatfield D, Atkins JF, Ban N. Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome. Science. 2021 Jun 18;372(6548):1306-1313. PMID:34029205
The pseudoknot at the entry to the mRNA channel is a key structural characteristic for translation of the SARS-CoV-2
RNA
genome. It specifically interacts with ribosomal proteins (Rabbit 80S ribosome) and 18S rRNA and causes ribosomal pausing prior to -1 frameshifting and the translating ribosome structure was studied by cryo-electron microscopy to a high resolution.
Interfering with the frameshifting process at the level of nascent chain interactions with the ribosomal tunnel at the level of RNA folding leads to the formation of the frameshift stimulatory pseudoknot, representing a viable strategy in the search for new drugs against SARS-CoV-2.
✍
34029205
(
Science
)
PMID
34029205
Date of Publishing
: 2021 Jun 18
Title
Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome
Author(s) name
Bhatt PR, Scaiola A et al.
Journal
Science
Impact factor
20.57
Citation count
: 51
Date of Entry
2021 Aug 11
×
NLM format
Bhatt PR, Scaiola A, Loughran G, Leibundgut M, Kratzel A, Meurs R, Dreos R, O'Connor KM, McMillan A, Bode JW, Thiel V, Gatfield D, Atkins JF, Ban N. Structural basis of ribosomal frameshifting during translation of the SARS-CoV-2 RNA genome. Science. 2021 Jun 18;372(6548):1306-1313. PMID:34029205
Monovalent hACE2 decoy CTC-445.2 binds to all the three RBDs of a single
spike protein
with a low nanomolar affinity and high specificity. The divalent CTC-445.2d shows about ~10 fold increase in the
binding.
De novo protein design approach to generate decoys is independent to traditional therapeutics and has the potential to better overcome mutational viral evasion.
✍
33154107
(
Science
)
PMID
33154107
Date of Publishing
: 2020 Dec 4
Title
De novo design of potent and resilient hACE2 decoys to neutralize SARS-CoV-2
Author(s) name
Linsky TW, Vergara R et al.
Journal
Science
Impact factor
20.57
Citation count
: 75
Date of Entry
2021 Jul 28
×
NLM format
Linsky TW, Vergara R, Codina N, Nelson JW, Walker MJ, Su W, Barnes CO, Hsiang TY, Esser-Nobis K, Yu K, Reneer ZB, Hou YJ, Priya T, Mitsumoto M, Pong A, Lau UY, Mason ML, Chen J, Chen A, Berrocal T, Peng H, Clairmont NS, Castellanos J, Lin YR, Josephson-Day A, Baric RS, Fuller DH, Walkey CD, Ross TM, Swanson R, Bjorkman PJ, Gale M Jr, Blancas-Mejia LM, Yen HL, Silva DA. De novo design of potent and resilient hACE2 decoys to neutralize SARS-CoV-2. Science. 2020 Dec 4;370(6521):1208-1214. PMID:33154107