Vinorelbine causes a neuropathic pain-like state in mice via STING and MNK1 signaling associated with type I interferon induction

Úrzula Franco-Enzástiga; Keerthana Natarajan; Eric T David; Krish Patel; Abhira Ravirala; Theodore J Price

doi:10.1016/j.isci.2024.108808

Vinorelbine causes a neuropathic pain-like state in mice via STING and MNK1 signaling associated with type I interferon induction

iScience. 2024 Jan 8;27(2):108808. doi: 10.1016/j.isci.2024.108808. eCollection 2024 Feb 16.

Authors

Úrzula Franco-Enzástiga¹, Keerthana Natarajan¹, Eric T David¹, Krish Patel¹, Abhira Ravirala¹, Theodore J Price¹

Affiliation

¹ Center for Advanced Pain Studies, School of Behavioral and Brain Sciences, University of Texas at Dallas, Richardson, TX 75080, USA.

Abstract

Type I interferons (IFNs) increase the excitability of dorsal root ganglia (DRGs) neurons via MNK-eIF4E signaling to promote pain sensitization in mice. Activation of stimulator of interferon response cGAMP interactor 1 (STING) signaling is pivotal for type I IFN induction. We hypothesized that vinorelbine, a chemotherapeutic and activator of STING, would cause a neuropathic pain-like state in mice via STING signaling in DRG neurons associated with IFN production. Vinorelbine caused tactile allodynia and grimacing in wild-type (WT) mice and increased p-IRF3, type I IFNs, and p-eIF4E in peripheral nerves. Supporting our hypothesis, vinorelbine failed to induce IRF3-IFNs-MNK-eIF4E in Sting^Gt/Gt mice and, subsequently, failed to cause pain. The vinorelbine-elicited increase of p-eIF4E was not observed in Mknk1^-/- (MNK1 knockout) mice in peripheral nerves consistent with the attenuated pro-nociceptive effect of vinorelbine in these mice. Our findings show that activation of STING signaling in the periphery causes a neuropathic pain-like state through type I IFN signaling to DRG nociceptors.

Keywords: Cellular neuroscience; Molecular neuroscience.

Grants and funding

R01 NS065926/NS/NINDS NIH HHS/United States