The inhibitory effect of inflammation and endotoxins on the secretion of reproductive hormones from the hypothalamo-pituitary axis is well documented. A comparison of the luteinizing hormone (LH) suppressing effects of several pro-inflammatory cytokines revealed that centrally administered IL-1β was the most potent inhibitor of pituitary LH secretion; interleukin (IL)-1α and tumor necrosis factor (TNF)α were relatively less effective, whereas IL-6 was ineffective. This order of potency suggested that the anti-gonadotropic effects of an immune challenge are most likely attributable to the action of centrally released IL-1β, and this was supported by the demonstration that IL-1β suppressed hypothalamic luteinizing hormone releasing hormone (LHRH) release. We used a multifaceted approach to identify the afferent signals in the brain that convey immune messages to hypothalamic LHRH neurons. Pharmacological studies with specific antagonists of opioid receptor subtypes demonstrated that activation of the μ1 receptor subtype was required to transmit the cytokine signal. Furthermore, icv IL-1β upregulated hypothalamic POMC mRNA and increased the concentration and release of β-endorphin, the primary ligand of μ1 receptors. We have obtained evidence that IL-1β also enhanced the gene expression and concentration of tachykinins, a family of nociceptive neuropeptides in the hypothalamus. Blockade of tachykinergic NK2 receptors attenuated IL-1β induced inhibition of LH secretion. Collectively, these results demonstrate that IL-1β, generated centrally in response to inflammation, upregulates the opioid and tachykinin peptides in the hypothalamus. These two groups of neuropeptides are critically involved in relaying the cytokine signal to neuroendocrine neurons and causing the suppression of hypothalamic LHRH and pituitary LH release.