SLIRP promotes autoimmune diseases by amplifying antiviral signaling via positive feedback regulation

bioRxiv [Preprint]. 2024 Jun 10:2024.03.28.587146. doi: 10.1101/2024.03.28.587146.

Abstract

The abnormal innate immune response is a prominent feature underlying autoimmune diseases. One emerging factor that can trigger dysregulated immune activation is cytosolic mitochondrial double-stranded RNAs (mt-dsRNAs). However, the mechanism by which mt-dsRNAs stimulate immune responses remains poorly understood. Here, we discover SRA stem-loop interacting RNA binding protein (SLIRP) as a key amplifier of mt-dsRNA-triggered antiviral signals. In autoimmune diseases, SLIRP is commonly upregulated, and targeted knockdown of SLIRP dampens the interferon response. We find that the activation of melanoma differentiation-associated gene 5 (MDA5) by exogenous dsRNAs upregulates SLIRP, which then stabilizes mt-dsRNAs and promotes their cytosolic release to activate MDA5 further, augmenting the interferon response. Furthermore, the downregulation of SLIRP partially rescues the abnormal interferon-stimulated gene expression in autoimmune patients' primary cells and makes cells vulnerable to certain viral infections. Our study unveils SLIRP as a pivotal mediator of interferon response through positive feedback amplification of antiviral signaling.

Keywords: Double-stranded RNAs; SLIRP; Sjögren’s disease; antiviral signaling; autoimmune disease; innate immune response; interferon response; mitochondrial RNAs; mitochondrial-nuclear communication; viral infection.

Publication types

  • Preprint