Prostaglandin-dependent modulation of dopaminergic neurotransmission elicits inflammation-induced aversion in mice
Michael Fritz, … , Anders Blomqvist, David Engblom
Michael Fritz, … , Anders Blomqvist, David Engblom
Published February 1, 2016; First published December 21, 2015
Citation Information: J Clin Invest. 2016;126(2):695-705. https://doi.org/10.1172/JCI83844.
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Categories: Research Article Neuroscience

Prostaglandin-dependent modulation of dopaminergic neurotransmission elicits inflammation-induced aversion in mice

Abstract

Systemic inflammation causes malaise and general feelings of discomfort. This fundamental aspect of the sickness response reduces the quality of life for people suffering from chronic inflammatory diseases and is a nuisance during mild infections like common colds or the flu. To investigate how inflammation is perceived as unpleasant and causes negative affect, we used a behavioral test in which mice avoid an environment that they have learned to associate with inflammation-induced discomfort. Using a combination of cell-type–specific gene deletions, pharmacology, and chemogenetics, we found that systemic inflammation triggered aversion through MyD88-dependent activation of the brain endothelium followed by COX1-mediated cerebral prostaglandin E2 (PGE2) synthesis. Further, we showed that inflammation-induced PGE2 targeted EP1 receptors on striatal dopamine D1 receptor–expressing neurons and that this signaling sequence induced aversion through GABA-mediated inhibition of dopaminergic cells. Finally, we demonstrated that inflammation-induced aversion was not an indirect consequence of fever or anorexia but that it constituted an independent inflammatory symptom triggered by a unique molecular mechanism. Collectively, these findings demonstrate that PGE2-mediated modulation of the dopaminergic motivational circuitry is a key mechanism underlying the negative affect induced by inflammation.

Authors

Michael Fritz, Anna M. Klawonn, Anna Nilsson, Anand Kumar Singh, Joanna Zajdel, Daniel Björk Wilhelms, Michael Lazarus, Andreas Löfberg, Maarit Jaarola, Unn Örtegren Kugelberg, Timothy R. Billiar, David J. Hackam, Chhinder P. Sodhi, Matthew D. Breyer, Johan Jakobsson, Markus Schwaninger, Günther Schütz, Jan Rodriguez Parkitna, Clifford B. Saper, Anders Blomqvist, David Engblom

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Figure 5

Inflammation induces aversion by inhibiting dopaminergic signaling.

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Inflammation induces aversion by inhibiting dopaminergic signaling. (A a...
(A and B) Recombination induced by the Dat Cre-ERT2 line. Recombination is specific to tyrosine hydroxylase–positive (TH-positive) dopaminergic cells. (C) Inflammatory aversion is blocked in mice lacking GABAA receptor γ 2 subunits (Gabrg2 Dat Cre-ERT2; n = 7, WT; 7, Gabrg2 Dat Cre-ERT2 ). (D) Ep1r KO mice do not display inflammation-induced aversion but develop place avoidance if a D1R antagonist is administered i.p. prior to LPS training (n = 6, Ep1r KO; 5, Ep1r KO + D1R antagonist). (E) DREADD-Gq expression in the midbrain of Dat Cre-ERT2 mice (immunofluorescent detection of mCherry fused to the receptors). (F) Aversion scores in WT and Dat Cre-ERT2 mice injected with a Cre-dependent Gq-DREADD–expressing viral vector and injected i.p. with CNO before LPS training (n = 7, WT; 5, Dat Cre Dio-DREADD). Scale bars: 200 μm (A and E) and 25 μm (B). **P < 0.01, Student’s t test.