CC chemokine ligand-2 synergizes with the nonchemokine G protein-coupled receptor ligand fMLP in monocyte chemotaxis, and it cooperates with the TLR ligand LPS via induction of CXCL8

Mieke Gouwy^*, Sofie Struyf^*, Hannelien Verbeke^*, Willy Put^*, Paul Proost^*, Ghislain Opdenakker and Jo Van Damme^*^,1

^* Laboratory of Molecular Immunology and
Laboratory of Immunobiology, Rega Institute for Medical Research, University of Leuven, Leuven, Belgium

1. Correspondence: Laboratory of Molecular Immunology, Rega Institute, Minderbroedersstraat 10, B-3000 Leuven, Belgium. E-mail: jo.vandamme{at}rega.kuleuven.be

ABSTRACT

During inflammatory reactions, endogenously produced cytokinesand chemokines act in a network and interact with hormones andneurotransmitters to regulate host immune responses. These signalingcircuitries are even more interfaced during infections, whenmicrobial agonists activate TLR, RLR, and NLR receptors. Onthe basis of the discovery of synergy between chemokines forneutrophil attraction, we extend here this phenomenon betweenthe chemokine MCP-1/CCL2 and the GPCR ligand fMLP or the TLR4agonist LPS on monocytes. In fact, the bacterial tripeptidefMLP, but not the cytokines IL-1β or IFN- ${gamma}$ , significantlyand dose-dependently synergized with CCL2 in monocyte chemotaxis.Furthermore, LPS rapidly induced the expression of IL-8/CXCL8but not of the CCL2 receptor CCR2 in monocytic cells. In turn,the induced CXCL8 synergized with CCL2 for mononuclear cellchemotaxis, and the chemotactic effect was mediated by CXCR1/CXCR2,because CXCL8 receptor antagonists or antibodies were capableof blocking the synergy, while keeping the responsiveness toCCL2 intact. These data recapitulate in vitro the complexityof innate immune regulation, provide a novel mechanism of enhancingmonocyte chemotaxis during bacterial infections with gram-negativebacteria and demonstrate the importance of local contexts ininflammatory and infectious insults.

Key Words: chemokines • migration • cytokines