Your search keyword '"Pyo, Chul-Woo"' showing total 5 results

1. Rare, convergent antibodies targeting the stem helix broadly neutralize diverse betacoronaviruses.

Author

Dacon C, Peng L, Lin TH, Tucker C, Lee CD, Cong Y, Wang L, Purser L, Cooper AJR, Williams JK, Pyo CW, Yuan M, Kosik I, Hu Z, Zhao M, Mohan D, Peterson M, Skinner J, Dixit S, Kollins E, Huzella L, Perry D, Byrum R, Lembirik S, Murphy M, Zhang Y, Yang ES, Chen M, Leung K, Weinberg RS, Pegu A, Geraghty DE, Davidson E, Doranz BJ, Douagi I, Moir S, Yewdell JW, Schmaljohn C, Crompton PD, Mascola JR, Holbrook MR, Nemazee D, Wilson IA, and Tan J

Subjects

Animals, Cricetinae, Antibodies, Monoclonal, Disease Outbreaks, Mesocricetus, Antibodies, Viral, Antibodies, Neutralizing, Spike Glycoprotein, Coronavirus genetics, SARS-CoV-2, COVID-19

Abstract

Humanity has faced three recent outbreaks of novel betacoronaviruses, emphasizing the need to develop approaches that broadly target coronaviruses. Here, we identify 55 monoclonal antibodies from COVID-19 convalescent donors that bind diverse betacoronavirus spike proteins. Most antibodies targeted an S2 epitope that included the K814 residue and were non-neutralizing. However, 11 antibodies targeting the stem helix neutralized betacoronaviruses from different lineages. Eight antibodies in this group, including the six broadest and most potent neutralizers, were encoded by IGHV1-46 and IGKV3-20. Crystal structures of three antibodies of this class at 1.5-1.75-Å resolution revealed a conserved mode of binding. COV89-22 neutralized SARS-CoV-2 variants of concern including Omicron BA.4/5 and limited disease in Syrian hamsters. Collectively, these findings identify a class of IGHV1-46/IGKV3-20 antibodies that broadly neutralize betacoronaviruses by targeting the stem helix but indicate these antibodies constitute a small fraction of the broadly reactive antibody response to betacoronaviruses after SARS-CoV-2 infection., Competing Interests: Declaration of interests J.T. and C.D. are co-inventors on a provisional patent (US Patent application no. 63/308,898) filed on the mAbs described in this study. J.K.W., E.D., and B.J.D. are employees of Integral Molecular; B.J.D. is a shareholder in this company. Y.C., S.D., E.K., L.H., D.L.P., R.B., S.L., and M.R.H. performed this work as employees of Laulima Government Solutions, LLC. M.M. performed this work as an employee of Tunnell Government Services, Inc., a subcontractor to Laulima Government Solutions, LLC. The content of this publication does not necessarily reflect the views or policies of the DHHS or of the institutions and companies with which the authors are affiliated. All other authors declare no competing interests., (Published by Elsevier Inc.)

Published

2023

2. Rapidly identifying new coronavirus mutations of potential concern in the Omicron variant using an unsupervised learning strategy.

Author

Zhao LP, Lybrand TP, Gilbert PB, Payne TH, Pyo CW, Geraghty DE, and Jerome KR

Subjects

Humans, Unsupervised Machine Learning, SARS-CoV-2 genetics, RNA-Dependent RNA Polymerase, Mutation, Phosphoproteins genetics, Spike Glycoprotein, Coronavirus genetics, COVID-19 epidemiology, COVID-19 genetics

Abstract

Extensive mutations in the Omicron spike protein appear to accelerate the transmission of SARS-CoV-2, and rapid infections increase the odds that additional mutants will emerge. To build an investigative framework, we have applied an unsupervised machine learning approach to 4296 Omicron viral genomes collected and deposited to GISAID as of December 14, 2021, and have identified a core haplotype of 28 polymutants (A67V, T95I, G339D, R346K, S371L, S373P, S375F, K417N, N440K, G446S, S477N, T478K, E484A, Q493R, G496S, Q498R, N501Y, Y505H, T547K, D614G, H655Y, N679K, P681H, N764K, K796Y, N856K, Q954H, N69K, L981F) in the spike protein and a separate core haplotype of 17 polymutants in non-spike genes: (K38, A1892) in nsp3, T492 in nsp4, (P132, V247, T280, S284) in 3C-like proteinase, I189 in nsp6, P323 in RNA-dependent RNA polymerase, I42 in Exonuclease, T9 in envelope protein, (D3, Q19, A63) in membrane glycoprotein, and (P13, R203, G204) in nucleocapsid phosphoprotein. Using these core haplotypes as reference, we have identified four newly emerging polymutants (R346, A701, I1081, N1192) in the spike protein (p value = 9.37*10 -4 , 1.0*10 -15 , 4.76*10 -7 and 1.56*10 -4 , respectively), and five additional polymutants in non-spike genes (D343G in nucleocapsid phosphoprotein, V1069I in nsp3, V94A in nsp4, F694Y in the RNA-dependent RNA polymerase and L106L/F of ORF3a) that exhibit significant increasing trajectories (all p values < 1.0*10 -15 ). In the absence of relevant clinical data for these newly emerging mutations, it is important to monitor them closely. Two emerging mutations may be of particular concern: the N1192S mutation in spike protein locates in an extremely highly conserved region of all human coronaviruses that is integral to the viral fusion process, and the F694Y mutation in the RNA polymerase may induce conformational changes that could impact remdesivir binding., (© 2022. The Author(s).)

Published

2022

3. Broadly neutralizing antibodies target the coronavirus fusion peptide.

Author

Dacon C, Tucker C, Peng L, Lee CD, Lin TH, Yuan M, Cong Y, Wang L, Purser L, Williams JK, Pyo CW, Kosik I, Hu Z, Zhao M, Mohan D, Cooper AJR, Peterson M, Skinner J, Dixit S, Kollins E, Huzella L, Perry D, Byrum R, Lembirik S, Drawbaugh D, Eaton B, Zhang Y, Yang ES, Chen M, Leung K, Weinberg RS, Pegu A, Geraghty DE, Davidson E, Douagi I, Moir S, Yewdell JW, Schmaljohn C, Crompton PD, Holbrook MR, Nemazee D, Mascola JR, Wilson IA, and Tan J

Subjects

COVID-19 Vaccines chemistry, COVID-19 Vaccines immunology, Humans, Peptides immunology, Protein Conformation, alpha-Helical, Protein Domains, Antibodies, Monoclonal immunology, Antibodies, Viral immunology, Broadly Neutralizing Antibodies immunology, COVID-19 immunology, COVID-19 prevention & control, Epitopes chemistry, Epitopes immunology, SARS-CoV-2 immunology, Spike Glycoprotein, Coronavirus chemistry, Spike Glycoprotein, Coronavirus immunology

Abstract

The potential for future coronavirus outbreaks highlights the need to broadly target this group of pathogens. We used an epitope-agnostic approach to identify six monoclonal antibodies that bind to spike proteins from all seven human-infecting coronaviruses. All six antibodies target the conserved fusion peptide region adjacent to the S2' cleavage site. COV44-62 and COV44-79 broadly neutralize alpha- and betacoronaviruses, including severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) Omicron subvariants BA.2 and BA.4/5, albeit with lower potency than receptor binding domain-specific antibodies. In crystal structures of COV44-62 and COV44-79 antigen-binding fragments with the SARS-CoV-2 fusion peptide, the fusion peptide epitope adopts a helical structure and includes the arginine residue at the S2' cleavage site. COV44-79 limited disease caused by SARS-CoV-2 in a Syrian hamster model. These findings highlight the fusion peptide as a candidate epitope for next-generation coronavirus vaccine development.

Published

2022

4. Mutations in viral nucleocapsid protein and endoRNase are discovered to associate with COVID19 hospitalization risk.

Author

Zhao LP, Roychoudhury P, Gilbert P, Schiffer J, Lybrand TP, Payne TH, Randhawa A, Thiebaud S, Mills M, Greninger A, Pyo CW, Wang R, Li R, Thomas A, Norris B, Nelson WC, Jerome KR, and Geraghty DE

Subjects

Female, Humans, Male, Washington epidemiology, COVID-19 epidemiology, COVID-19 genetics, COVID-19 therapy, Haplotypes, Hospitalization, Mutation, SARS-CoV-2 genetics

Abstract

SARS-CoV-2 is spreading worldwide with continuously evolving variants, some of which occur in the Spike protein and appear to increase viral transmissibility. However, variants that cause severe COVID-19 or lead to other breakthroughs have not been well characterized. To discover such viral variants, we assembled a cohort of 683 COVID-19 patients; 388 inpatients ("cases") and 295 outpatients ("controls") from April to August 2020 using electronically captured COVID test request forms and sequenced their viral genomes. To improve the analytical power, we accessed 7137 viral sequences in Washington State to filter out viral single nucleotide variants (SNVs) that did not have significant expansions over the collection period. Applying this filter led to the identification of 53 SNVs that were statistically significant, of which 13 SNVs each had 3 or more variant copies in the discovery cohort. Correlating these selected SNVs with case/control status, eight SNVs were found to significantly associate with inpatient status (q-values < 0.01). Using temporal synchrony, we identified a four SNV-haplotype (t19839-g28881-g28882-g28883) that was significantly associated with case/control status (Fisher's exact p = 2.84 × 10 -11 ). This haplotype appeared in April 2020, peaked in June, and persisted into January 2021. The association was replicated (OR = 5.46, p-value = 4.71 × 10 -12 ) in an independent cohort of 964 COVID-19 patients (June 1, 2020 to March 31, 2021). The haplotype included a synonymous change N73N in endoRNase, and three non-synonymous changes coding residues R203K, R203S and G204R in the nucleocapsid protein. This discovery points to the potential functional role of the nucleocapsid protein in triggering "cytokine storms" and severe COVID-19 that led to hospitalization. The study further emphasizes a need for tracking and analyzing viral sequences in correlations with clinical status., (© 2022. The Author(s).)

Published

2022

5. Author Correction: Mutations in viral nucleocapsid protein and endoRNase are discovered to associate with COVID19 hospitalization risk.

Author

Zhao, Lue Ping, Roychoudhury, Pavitra, Gilbert, Peter, Schiffer, Joshua, Lybrand, Terry P., Payne, Thomas H., Randhawa, April, Thiebaud, Sara, Mills, Margaret, Greninger, Alex, Pyo, Chul-Woo, Wang, Ruihan, Li, Renyu, Thomas, Alexander, Norris, Brandon, Nelson, Wyatt C., Jerome, Keith R., and Geraghty, Daniel E.

Subjects

VIRAL mutation, VIRAL proteins, COVID-19, VIRAL genomes, HOSPITAL care

Abstract

Correction to: I Scientific Reports i https://doi.org/10.1038/s41598-021-04376-4, published online 24 January 2022 The original version of this Article contained an error in Figure 1, where an old version of the figure was mistakenly submitted for publication. These authors contributed equally: Lue Ping Zhao and Pavitra Roychoudhury. [Extracted from the article]

Published

2022