Berbamine suppresses intestinal SARS-CoV-2 infection via a BNIP3-dependent autophagy blockade

Alexandra P M Cloherty; Anusca G Rader; Kharishma S Patel; Jimena Pérez-Vargas; Connor A H Thompson; Siobhan Ennis; Masahiro Niikura; Manon E Wildenberg; Vanesa Muncan; Renée R C E Schreurs; François Jean; Carla M S Ribeiro

doi:10.1080/22221751.2023.2195020

Berbamine suppresses intestinal SARS-CoV-2 infection via a BNIP3-dependent autophagy blockade

Emerg Microbes Infect. 2023 Dec;12(1):2195020. doi: 10.1080/22221751.2023.2195020.

Authors

Alexandra P M Cloherty^{1

2}, Anusca G Rader^{1

2

3}, Kharishma S Patel^{1

2}, Jimena Pérez-Vargas⁴, Connor A H Thompson⁴, Siobhan Ennis⁵, Masahiro Niikura⁵, Manon E Wildenberg^{3

6}, Vanesa Muncan^{3

6}, Renée R C E Schreurs^{1

2

3}, François Jean⁴, Carla M S Ribeiro^{1

2

3}

Affiliations

¹ Department of Experimental Immunology, Amsterdam UMC, University of Amsterdam, Amsterdam, The Netherlands.
² Infectious Diseases & Inflammatory Diseases Programs, Amsterdam Institute for Infection & Immunity, Amsterdam, The Netherlands.
³ Amsterdam Gastroenterology & Metabolism, University of Amsterdam, Amsterdam, The Netherlands.
⁴ Department of Microbiology and Immunology, Life Sciences Institute, University of British Columbia, Vancouver, Canada.
⁵ Faculty of Health Sciences, Simon Fraser University, Burnaby, Canada.
⁶ Amsterdam Gastroenterology Endocrinology and Metabolism, Tytgat institute for Intestinal and Liver research, Amsterdam UMC, University of Amsterdam, Amsterdam, The Netherlands.

Abstract

SARS-CoV-2, the causative virus of COVID-19, continues to threaten global public health. COVID-19 is a multi-organ disease, causing not only respiratory distress, but also extrapulmonary manifestations, including gastrointestinal symptoms with SARS-CoV-2 RNA shedding in stool long after respiratory clearance. Despite global vaccination and existing antiviral treatments, variants of concern are still emerging and circulating. Of note, new Omicron BA.5 sublineages both increasingly evade neutralizing antibodies and demonstrate an increased preference for entry via the endocytic entry route. Alternative to direct-acting antivirals, host-directed therapies interfere with host mechanisms hijacked by viruses, and enhance cell-mediated resistance with a reduced likelihood of drug resistance development. Here, we demonstrate that the autophagy-blocking therapeutic berbamine dihydrochloride robustly prevents SARS-CoV-2 acquisition by human intestinal epithelial cells via an autophagy-mediated BNIP3 mechanism. Strikingly, berbamine dihydrochloride exhibited pan-antiviral activity against Omicron subvariants BA.2 and BA.5 at nanomolar potency, providing a proof of concept for the potential for targeting autophagy machinery to thwart infection of current circulating SARS-CoV-2 subvariants. Furthermore, we show that autophagy-blocking therapies limited virus-induced damage to intestinal barrier function, affirming the therapeutic relevance of autophagy manipulation to avert the intestinal permeability associated with acute COVID-19 and post-COVID-19 syndrome. Our findings underscore that SARS-CoV-2 exploits host autophagy machinery for intestinal dissemination and indicate that repurposed autophagy-based antivirals represent a pertinent therapeutic option to boost protection and ameliorate disease pathogenesis against current and future SARS-CoV-2 variants of concern.

Keywords: Human intestinal organoids; Intestinal barrier function; Intestinal damage; Viral entry routes; autophagy; drug repurposing; extrapulmonary COVID-19; host-directed antiviral therapy.

MeSH terms

Antibodies, Neutralizing
Antibodies, Viral
Antiviral Agents / pharmacology
Autophagy
COVID-19*
Hepatitis C, Chronic*
Humans
Membrane Proteins
Post-Acute COVID-19 Syndrome
RNA, Viral
SARS-CoV-2
Spike Glycoprotein, Coronavirus

Substances

berbamine
Antiviral Agents
RNA, Viral
Antibodies, Neutralizing
Antibodies, Viral
Spike Glycoprotein, Coronavirus
spike protein, SARS-CoV-2
BNIP3 protein, human
Membrane Proteins

Supplementary concepts

SARS-CoV-2 variants

Grants and funding

This work was funded by AMC PhD Scholarship and Amsterdam UMC grant (awarded to APMC and CMSR), Dutch Research Council (NWO-ZonMw) VIDI grant 91718331 and ASPASIA grant 015.014.030 (both awarded to CMSR), Coronavirus Variants Rapid Response Network (CoVaRR-Net) research grant #175622 (awarded to FJ), and by an Amsterdam institute for Infection & Immunity COVID-19 Grant (awarded to CMSR, MW, VM, and FJ).