The Antiviral Activity of the Lectin Griffithsin against SARS-CoV-2 Is Enhanced by the Presence of Structural Proteins
Author:
Bains Arjan1ORCID, Fischer Kathryn2, Guan Wenyan3ORCID, LiWang Patricia J.4ORCID
Affiliation:
1. Chemistry and Biochemistry, University of California Merced, 5200 North Lake Rd., Merced, CA 95343, USA 2. Quantitative and Systems Biology, University of California Merced, 5200 North Lake Rd., Merced, CA 95343, USA 3. Materials and Biomaterials Science and Engineering, University of California Merced, 5200 North Lake Rd., Merced, CA 95343, USA 4. Molecular Cell Biology, Health Sciences Research Institute, University of California Merced, 5200 North Lake Rd., Merced, CA 95343, USA
Abstract
Although COVID-19 transmission has been reduced by the advent of vaccinations and a variety of rapid monitoring techniques, the SARS-CoV-2 virus itself has shown a remarkable ability to mutate and persist. With this long track record of immune escape, researchers are still exploring prophylactic treatments to curtail future SARS-CoV-2 variants. Specifically, much focus has been placed on the antiviral lectin Griffithsin in preventing spike protein-mediated infection via the hACE2 receptor (direct infection). However, an oft-overlooked aspect of SARS-CoV-2 infection is viral capture by attachment receptors such as DC-SIGN, which is thought to facilitate the initial stages of COVID-19 infection in the lung tissue (called trans-infection). In addition, while immune escape is dictated by mutations in the spike protein, coronaviral virions also incorporate M, N, and E structural proteins within the particle. In this paper, we explored how several structural facets of both the SARS-CoV-2 virion and the antiviral lectin Griffithsin can affect and attenuate the infectivity of SARS-CoV-2 pseudovirus. We found that Griffithsin was a better inhibitor of hACE2-mediated direct infection when the coronaviral M protein is present compared to when it is absent (possibly providing an explanation regarding why Griffithsin shows better inhibition against authentic SARS-CoV-2 as opposed to pseudotyped viruses, which generally do not contain M) and that Griffithsin was not an effective inhibitor of DC-SIGN-mediated trans-infection. Furthermore, we found that DC-SIGN appeared to mediate trans-infection exclusively via binding to the SARS-CoV-2 spike protein, with no significant effect observed when other viral proteins (M, N, and/or E) were present. These results provide etiological data that may help to direct the development of novel antiviral treatments, either by leveraging Griffithsin binding to the M protein as a novel strategy to prevent SARS-CoV-2 infection or by narrowing efforts to inhibit trans-infection to focus on DC-SIGN binding to SARS-CoV-2 spike protein.
Funder
Army Research Office NSF-CREST Center for Cellular and Biomolecular Machines COVID-19 funding program of the Health Science Research Institute at U.C. Merced
Subject
Virology,Infectious Diseases
Reference110 articles.
1. (2023, August 25). WHO Coronavirus (COVID-19) Dashboard. Available online: https://covid19.who.int/. 2. Zabidi, N.Z., Liew, H.L., Farouk, I.A., Puniyamurti, A., Yip, A.J.W., Wijesinghe, V.N., Low, Z.Y., Tang, J.W., Chow, V.T.K., and Lal, S.K. (2023). Evolution of SARS-CoV-2 Variants: Implications on Immune Escape, Vaccination, Therapeutic and Diagnostic Strategies. Viruses, 15. 3. Impact of vaccination on the COVID-19 pandemic in U.S. states;Chen;Sci. Rep.,2022 4. (2023, July 29). CDC Covid Data Tracker, Available online: https://covid.cdc.gov/covid-data-tracker/#datatracker-home. 5. mRNA vaccine-elicited antibodies to SARS-CoV-2 and circulating variants;Wang;Nature,2021
|
|