g , exploratory, anxiety, sickness) are regulated by different me

g., exploratory, anxiety, sickness) are regulated by different mediators. We show that the drugs tested in our study all reduced the hypothermic response to a systemic challenge of LPS, inhibited COX-2 expression in the hippocampus and inhibited PGE2 levels in the hypothalamus. Furthermore, COX-2 selective inhibitors potently inhibit LPS-induced IL-1β, IL-6 and TNF-α levels in the brain. These results are in accordance mTOR inhibitor with well-accepted studies using selective pharmacological

inhibitors and knockout mice that proved that the febrile response and behavioural changes induced by IL-1β, depend on COX-2 (Blatteis, 2007, Romanovsky et al., 2005 and Zhang and Rivest, 2001). There are also studies showing that pharmacological cytokine inhibitors, for example dexamethasone are less effective against LPS-induced behavioural changes as compared to IL-1β-induced changes (Dunn and Swiergiel, 2000), and mPGES-1 deficient mice are not different to wild-type mice when challenged with LPS, while protected from IL-1β-induced anorexia (Pecchi et al., 2006). These studies strongly suggest that, cytokines and PGE2 have different effects

Selleckchem Galunisertib on brain functions and/or act on different regions in the brain. Interestingly, Zhang et al. found a differential role for COX-1 and COX-2 in inducing fever and c-Fos expression, a marker for neuronal activity (Zhang et al., 2006 and Zhang et al., 2003). The COX-2 inhibitor SC-236

attenuated LPS-induced neuronal activity in specific forebrain sites including the ventromedial preoptic nucleus (VMPO) and the hypothalamic paraventricular nucleus (PVN), but not in brainstem sites Evodiamine such as the ventrolateral medulla (VLM), parabranchial nucleus (PB) and the nucleus of the solitary tract (NTS). The COX-1 inhibitor SC-560 showed the opposite effect, and blocked LPS-induced neuronal activity in the PVN, PB, NTS and VLM, without affecting the VMPO. The effects of systemic inflammation on brain activity are therefore not entirely dependent on COX-2 and certain responses may be regulated by COX-1. Based on these and our own results, we hypothesize that COX-2 and cytokine-mediated behaviour changes are functionally linked, while COX-1 mediated behavioural changes may occur independent of cytokines. It is worth mentioning that although dexamethasone-treated mice appeared normal and healthy, burrowing and open field were impaired after LPS challenge. These observations suggest that dexamethasone protects against classic sickness behaviours, but not behaviours associated with exploration and anxiety. In conclusion, using a mouse model for acute systemic inflammation in otherwise healthy mice, we have shown that pharmacologic blockade of COX-1 activity results in a complete reversal of LPS-induced deficits in burrowing and open-field activity.

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