Human Monocyte Recognition of Adenosine-Based Cyclic Dinucleotides Unveils the A2a G αs Protein-Coupled Receptor Tonic Inhibition of Mitochondrially Induced Cell Death

Author:

Tosolini Marie12345ORCID,Pont Frédéric12,Bétous Delphine12345,Ravet Emmanuel6,Ligat Laetitia12,Lopez Frédéric12,Poupot Mary12345,Poirot Marc12,Pérouzel Éric6,Tiraby Gérard6,Verhoeyen Els78,Fournié Jean-Jacques12345

Affiliation:

1. INSERM UMR1037, Centre Recherches en Cancérologie de Toulouse, Toulouse, France

2. Université Toulouse III Paul-Sabatier, Toulouse, France

3. ERL 5294 CNRS, Hôpital Purpan, Toulouse, France

4. Laboratoire d'Excellence TOUCAN, Toulouse, France

5. Institut Carnot CALYM, Pierre-Benite, France

6. Cayla-InVivoGen, Montaudran, France

7. CIRI, EVIR team, INSERM U1111, CNRS UMR5308, Université de Lyon-1, ENS de Lyon, Lyon, France

8. INSERM U1065, Centre Méditerranéen de Médecine Moléculaire, Nice, France

Abstract

ABSTRACT Cyclic dinucleotides are important messengers for bacteria and protozoa and are well-characterized immunity alarmins for infected mammalian cells through intracellular binding to STING receptors. We sought to investigate their unknown extracellular effects by adding cyclic dinucleotides to the culture medium of freshly isolated human blood cells in vitro . Here we report that adenosine-containing cyclic dinucleotides induce the selective apoptosis of monocytes through a novel apoptotic pathway. We demonstrate that these compounds are inverse agonist ligands of A2a, a G αs -coupled adenosine receptor selectively expressed by monocytes. Inhibition of monocyte A2a by these ligands induces apoptosis through a mechanism independent of that of the STING receptors. The blockade of basal (adenosine-free) signaling from A2a inhibits protein kinase A (PKA) activity, thereby recruiting cytosolic p53, which opens the mitochondrial permeability transition pore and impairs mitochondrial respiration, resulting in apoptosis. A2a antagonists and inverse agonist ligands induce apoptosis of human monocytes, while A2a agonists are antiapoptotic. In vivo , we used a mock developing human hematopoietic system through NSG mice transplanted with human CD34 + cells. Treatment with cyclic di-AMP selectively depleted A2a-expressing monocytes and their precursors via apoptosis. Thus, monocyte recognition of cyclic dinucleotides unravels a novel proapoptotic pathway: the A2a G αs protein-coupled receptor (GPCR)-driven tonic inhibitory signaling of mitochondrion-induced cell death.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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