Litcius/Paper detail

Chimeric GPCRs mimic distinct signaling pathways and modulate microglia responses

Rouven Schulz, Medina Korkut-Demirbaş, Alessandro Venturino, Gloria Colombo, Sandra Siegert

2022Nature Communications27 citationsDOIOpen Access PDF

Abstract

G protein-coupled receptors (GPCRs) regulate processes ranging from immune responses to neuronal signaling. However, ligands for many GPCRs remain unknown, suffer from off-target effects or have poor bioavailability. Additionally, dissecting cell type-specific responses is challenging when the same GPCR is expressed on different cells within a tissue. Here, we overcome these limitations by engineering DREADD-based GPCR chimeras that bind clozapine-N-oxide and mimic a GPCR-of-interest. We show that chimeric DREADD-β2AR triggers responses comparable to β2AR on second messenger and kinase activity, post-translational modifications, and protein-protein interactions. Moreover, we successfully recapitulate β2AR-mediated filopodia formation in microglia, an immune cell capable of driving central nervous system inflammation. When dissecting microglial inflammation, we included two additional DREADD-based chimeras mimicking microglia-enriched GPR65 and GPR109A. DREADD-β2AR and DREADD-GPR65 modulate the inflammatory response with high similarity to endogenous β2AR, while DREADD-GPR109A shows no impact. Our DREADD-based approach allows investigation of cell type-dependent pathways without known endogenous ligands.

Topics & Concepts

MicrogliaG protein-coupled receptorSignal transductionComputational biologyNeuroscienceBiologyCell biologyBioinformaticsInflammationImmunologyReceptor Mechanisms and SignalingNeuroinflammation and Neurodegeneration MechanismsNeuropeptides and Animal Physiology