| First Author | Pakai E | Year | 2018 |
| Journal | Front Immunol | Volume | 9 |
| Pages | 166 | PubMed ID | 29459872 |
| Mgi Jnum | J:337316 | Mgi Id | MGI:6869856 |
| Doi | 10.3389/fimmu.2018.00166 | Citation | Pakai E, et al. (2018) The Neurokinin-1 Receptor Contributes to the Early Phase of Lipopolysaccharide-Induced Fever via Stimulation of Peripheral Cyclooxygenase-2 Protein Expression in Mice. Front Immunol 9:166 |
| abstractText | Neurokinin (NK) signaling is involved in various inflammatory processes. A common manifestation of systemic inflammation is fever, which is usually induced in animal models with the administration of bacterial lipopolysaccharide (LPS). A role for the NK1 receptor was shown in LPS-induced fever, but the underlying mechanisms of how the NK1 receptor contributes to febrile response, especially in the early phase, have remained unknown. We administered LPS (120 microg/kg, intraperitoneally) to mice with the Tacr1 gene, i.e., the gene encoding the NK1 receptor, either present (Tacr1(+/+) ) or absent (Tacr1(-/-) ) and measured their thermoregulatory responses, serum cytokine levels, tissue cyclooxygenase-2 (COX-2) expression, and prostaglandin (PG) E2 concentration. We found that the LPS-induced febrile response was attenuated in Tacr1(-/-) compared to their Tacr1(+/+) littermates starting from 40 min postinfusion. The febrigenic effect of intracerebroventricularly administered PGE2 was not suppressed in the Tacr1(-/-) mice. Serum concentration of pyrogenic cytokines did not differ between Tacr1(-/-) and Tacr1(+/+) at 40 min post-LPS infusion. Administration of LPS resulted in amplification of COX-2 mRNA expression in the lungs, liver, and brain of the mice, which was statistically indistinguishable between the genotypes. In contrast, the LPS-induced augmentation of COX-2 protein expression was attenuated in the lungs and tended to be suppressed in the liver of Tacr1(-/-) mice compared with Tacr1(+/+) mice. The Tacr1(+/+) mice responded to LPS with a significant surge of PGE2 production in the lungs, whereas Tacr1(-/-) mice did not. In conclusion, the NK1 receptor is necessary for normal fever genesis. Our results suggest that the NK1 receptor contributes to the early phase of LPS-induced fever by enhancing COX-2 protein expression in the periphery. These findings advance the understanding of the crosstalk between NK signaling and the "cytokine-COX-2-prostaglandin E2" axis in systemic inflammation, thereby open up the possibilities for new therapeutic approaches. |
