Spying on SARS-CoV-2 with Fluorescent Tags and Protease Reporters

To, Tsz-Leung; Li, Xiaoquan; Shu, Xiaokun

Author(s)

To, Tsz-Leung; Li, Xiaoquan; Shu, Xiaokun

Downloadviruses-15-02005.pdf (1.621Mb)

Publisher with Creative Commons License

Terms of use

Creative Commons Attribution https://creativecommons.org/licenses/by/4.0/

Metadata

Show full item record

Abstract

The SARS-CoV-2 coronavirus has caused worldwide disruption through the COVID-19 pandemic, providing a sobering reminder of the profound impact viruses can have on human well-being. Understanding virus life cycles and interactions with host cells lays the groundwork for exploring therapeutic strategies against virus-related diseases. Fluorescence microscopy plays a vital role in virus imaging, offering high spatiotemporal resolution, sensitivity, and spectroscopic versatility. In this opinion piece, we first highlight two recent techniques, SunTag and StayGold, for the in situ imaging of viral RNA translation and viral assembly. Next, we discuss a new class of genetically encoded fluorogenic protease reporters, such as FlipGFP, which can be customized to monitor SARS-CoV-2’s main (M<sup>pro</sup>) or papain-like (PL<sup>pro</sup>) protease activity. These assays have proven effective in identifying potential antivirals through high-throughput screening, making fluorogenic viral protease reporters a promising platform for viral disease diagnostics and therapeutics.

Date issued

2023-09-27

URI

https://hdl.handle.net/1721.1/152530

Publisher

Multidisciplinary Digital Publishing Institute

Citation

Viruses 15 (10): 2005 (2023)

Version: Final published version

Collections

MIT Open Access Articles