SARS-CoV-2 Virus-like-particles Liposomal Reconstitution of Spike Glycoproteins

Overview

Journal Nanoscale Adv

Publisher Royal Society of Chemistry

Specialty Biotechnology

Date 2023 Aug 10

PMID 37560413

Authors

Sarah McColman

Klaidi Shkalla

Pavleen Sidhu

Jady Liang

Selena Osman

Norbert Kovacs

Zainab Bokhari

Ana Carolina Forjaz Marques

Yuchong Li

Qiwen Lin

Haibo Zhang

David T Cramb

Affiliations

Soon will be listed here.

Abstract

The SARS-CoV-2 virus, implicated in the COVID-19 pandemic, recognizes and binds host cells using its spike glycoprotein through an angiotensin converting enzyme 2 (ACE-2) receptor-mediated pathway. Recent research suggests that spatial distributions of the spike protein may influence viral interactions with target cells and immune systems. The goal of this study has been to develop a liposome-based virus-like particle (VLP) by reconstituting the SARS-CoV-2 spike glycoprotein within a synthetic nanoparticle membrane, aiming to eventually establish tunability in spike protein presentation on the nanoparticle surface. Here we report on first steps to this goal, wherein liposomal SARS-CoV-2 VLPs were successfully produced detergent mediated spike protein reconstitution. The resultant VLPs are shown to successfully co-localize with the ACE-2 receptor on lung epithelial cell surfaces, followed by internalization into these cells. These VLPs are the first step toward the overall goal of this research which is to form an understanding of the relationship between spike protein surface density and cell-level immune response, eventually toward creating better vaccines and anti-viral therapeutics.

Citing Articles

Dimming the corona: studying SARS-coronavirus-2 at reduced biocontainment level using replicons and virus-like particles.

Neilsen G, Mathew A, Castro J, McFadden W, Wen X, Ong Y mBio. 2024; 15(12):e0336823.

PMID: 39530689 PMC: 11633226. DOI: 10.1128/mbio.03368-23.

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