Nanobody-based pannexin1 channel inhibitors reduce inflammation in acute liver injury

Raf Van Campenhout; Timo W M De Groof; Prashant Kadam; Brenda R Kwak; Serge Muyldermans; Nick Devoogdt; Mathieu Vinken

doi:10.1186/s12951-023-02137-1

Nanobody-based pannexin1 channel inhibitors reduce inflammation in acute liver injury

J Nanobiotechnology. 2023 Oct 11;21(1):371. doi: 10.1186/s12951-023-02137-1.

Authors

Raf Van Campenhout^#¹, Timo W M De Groof^#², Prashant Kadam¹, Brenda R Kwak^{3

4}, Serge Muyldermans⁵, Nick Devoogdt^#², Mathieu Vinken^#⁶

Affiliations

¹ Entity of In Vitro Toxicology and Dermato-Cosmetology, Department of Pharmaceutical and Pharmacological Sciences, Vrije Universiteit Brussel, 1090, Brussels, Belgium.
² In Vivo Cellular and Molecular Imaging Laboratory, Department of Molecular Imaging, Vrije Universiteit Brussel, Laarbeeklaan 103, 1090, Brussels, Belgium.
³ Department of Pathology and Immunology, Faculty of Medicine, University of Geneva, CH-1211, Geneva, Switzerland.
⁴ Geneva Center for Inflammation Research, Faculty of Medicine, University of Geneva, CH-1211, Geneva, Switzerland.
⁵ Laboratory of Cellular and Molecular Immunology, Bioengineering Sciences Department, Vrije Universiteit Brussel, 1050, Brussels, Belgium.
⁶ Entity of In Vitro Toxicology and Dermato-Cosmetology, Department of Pharmaceutical and Pharmacological Sciences, Vrije Universiteit Brussel, 1090, Brussels, Belgium. mathieu.vinken@vub.be.

^# Contributed equally.

Abstract

Background: The opening of pannexin1 channels is considered as a key event in inflammation. Pannexin1 channel-mediated release of adenosine triphosphate triggers inflammasome signaling and activation of immune cells. By doing so, pannexin1 channels play an important role in several inflammatory diseases. Although pannexin1 channel inhibition could represent a novel clinical strategy for treatment of inflammatory disorders, therapeutic pannexin1 channel targeting is impeded by the lack of specific, potent and/or in vivo-applicable inhibitors. The goal of this study is to generate nanobody-based inhibitors of pannexin1 channels.

Results: Pannexin1-targeting nanobodies were developed as potential new pannexin1 channel inhibitors. We identified 3 cross-reactive nanobodies that showed affinity for both murine and human pannexin1 proteins. Flow cytometry experiments revealed binding capacities in the nanomolar range. Moreover, the pannexin1-targeting nanobodies were found to block pannexin1 channel-mediated release of adenosine triphosphate. The pannexin1-targeting nanobodies were also demonstrated to display anti-inflammatory effects in vitro through reduction of interleukin 1 beta amounts. This anti-inflammatory outcome was reproduced in vivo using a human-relevant mouse model of acute liver disease relying on acetaminophen overdosing. More specifically, the pannexin1-targeting nanobodies lowered serum levels of inflammatory cytokines and diminished liver damage. These effects were linked with alteration of the expression of several NLRP3 inflammasome components.

Conclusions: This study introduced for the first time specific, potent and in vivo-applicable nanobody-based inhibitors of pannexin1 channels. As demonstrated for the case of liver disease, the pannexin1-targeting nanobodies hold great promise as anti-inflammatory agents, yet this should be further tested for extrahepatic inflammatory disorders. Moreover, the pannexin1-targeting nanobodies represent novel tools for fundamental research regarding the role of pannexin1 channels in pathological and physiological processes.

Keywords: Acute liver disease; Inflammation; Nanobody; Pannexin1; Therapy.

MeSH terms

Adenosine Triphosphate
Animals
Anti-Inflammatory Agents
Humans
Inflammasomes
Inflammation / drug therapy
Liver Diseases*
Mice
Single-Domain Antibodies* / pharmacology
Single-Domain Antibodies* / therapeutic use

Substances

Adenosine Triphosphate
Anti-Inflammatory Agents
Inflammasomes
Single-Domain Antibodies

Grants and funding

Proof-of-Concept grant 861913/ERC_/European Research Council/International