Litcius/Paper detail

TRPV4 Inhibition and CRISPR-Cas9 Knockout Reduce Inflammation Induced by Hyperphysiological Stretching in Human Annulus Fibrosus Cells

Elena Cambria, Matthias Arlt, Sandra Wandel, Olga Krupková, Wolfgang Hitzl, Fabian S. Passini, Oliver Hausmann, Jess G. Snedeker, Stephen J. Ferguson, Karin Wuertz‐Kozak

2020Cells39 citationsDOIOpen Access PDF

Abstract

Mechanical loading and inflammation interact to cause degenerative disc disease and low back pain (LBP). However, the underlying mechanosensing and mechanotransductive pathways are poorly understood. This results in untargeted pharmacological treatments that do not take the mechanical aspect of LBP into account. We investigated the role of the mechanosensitive ion channel TRPV4 in stretch-induced inflammation in human annulus fibrosus (AF) cells. The cells were cyclically stretched to 20% hyperphysiological strain. TRPV4 was either inhibited with the selective TRPV4 antagonist GSK2193874 or knocked out (KO) via CRISPR-Cas9 gene editing. The gene expression, inflammatory mediator release and MAPK pathway activation were analyzed. Hyperphysiological cyclic stretching significantly increased the IL6, IL8, and COX2 mRNA, PGE2 release, and activated p38 MAPK. The TRPV4 pharmacological inhibition significantly attenuated these effects. TRPV4 KO further prevented the stretch-induced upregulation of IL8 mRNA and reduced IL6 and IL8 release, thus supporting the inhibition data. We provide novel evidence that TRPV4 transduces hyperphysiological mechanical signals into inflammatory responses in human AF cells, possibly via p38. Additionally, we show for the first time the successful gene editing of human AF cells via CRISPR-Cas9. The pharmacological inhibition or CRISPR-based targeting of TRPV4 may constitute a potential therapeutic strategy to tackle discogenic LBP in patients with AF injury.

Topics & Concepts

CRISPRTRPV4InflammationCell biologyCas9Mechanosensitive channelsMediatorProinflammatory cytokineDownregulation and upregulationp38 mitogen-activated protein kinasesChemistryMAPK/ERK pathwaySignal transductionBiologyTransient receptor potential channelIon channelImmunologyGeneReceptorBiochemistryMusculoskeletal pain and rehabilitationMyofascial pain diagnosis and treatmentSpine and Intervertebral Disc Pathology