Limbic progesterone receptor activity enhances neuronal excitability and seizures

Objective Emerging evidence raises the possibility that progesterone receptor (PR) signaling may contribute to the reproductive hormone fluctuation–linked seizure precipitation, called catamenial epilepsy. Therefore, we studied PR isoform expression in limbic regions involved in temporal lobe epilepsy and the effect of PR activation on neuronal activity and seizures. Methods We evaluated PR expression in the limbic regions, entorhinal cortex (EC), hippocampus, and amygdala in female rats using quantitative real‐time polymerase chain reaction (qRT‐PCR). A selective agonist, Nestorone (16‐methylene‐17 alpha‐acetoxy‐19‐nor‐pregn‐4‐ene‐3,20‐dione) activated PRs, and the effect on excitability and α‐amino‐3‐hydroxy‐5‐methyl‐4‐isoxazolepropionic acid receptor (AMPAR)–mediated synaptic transmission of EC neurons was studied using electrophysiology. Finally, we assessed PR regulation of epileptic seizures and status epilepticus (SE) induced by lithium‐pilocarpine in female rats with the global deletion of PRs (PR knockout; PRKO) using video electroencephalography (‐EEG). Results Limbic regions EC, hippocampus, and amygdala robustly expressed PR messenger RNA (mRNA). Nestorone (16‐methylene‐17 alpha‐acetoxy‐19‐nor‐pregn‐4‐ene‐3,20‐dione) treatment reduced the action potential threshold of layer II/III EC neurons and increased the frequency of AMPA receptor–mediated synaptic currents of ovariectomized and estrogen‐primed female rats. Female rats lacking PRs (PRKO) experienced a shorter duration, less intense, and less fatal SE than wild‐type (WT) animals. Furthermore, Nestorone treatment caused seizure exacerbation in the WT epileptic animals, but not in the PRKO epileptic animals. Significance Activation of PRs expressed in the EC and hippocampus increased neuronal excitability and worsened seizures. These receptors may play a role in catamenial epilepsy.