Objectives: A common experimental model of status epilepticus (SE) utilizes intraperitoneal administration of the cholinergic agonist pilocarpine preceded by methylscopolamine treatment. Currently, activation of cholinergic neurons is recognized as the only factor triggering pilocarpine SE. However, cholinergic receptors are also widely distributed systemically and pretreatment with methyl-scopolamine may not be sufficient to counteract the effects of systemically injected pilocarpine. The extent of such peripheral events and the contribution to SE are unknown and the possibility that pilocarpine also induces SE by peripheral actions is yet untested. Methods: We measured in vivo at onset of SE: brain and blood pilocarpine levels, blood-brain barrier (131313) permeability, T-lymphocyte activation and serum levels of IL-1 beta and TNF-alpha. The effects of pilocarpine on neuronal excitability was assessed in vitro on hippocampal slices or whole guinea pig brain preparations in presence of physiologic or elevated [K+](out). Results: Pilocarpine blood and brain levels at SE were 1400 +/- 200 mu M and 200 +/- 80 mu M, respectively. In vivo, after pilocarpine injection, increased serum IL-1 beta, decreased CD4:CD8 T-lymphocyte ratios and focal 131313 leakage were observed. In vitro, pilocarpine failed to exert significant synchronized epileptiform activity when applied at concentrations identical or higher to levels measured in vivo. Intense electrographic seizure-like events occurred only in the copresence of levels of K+ (6 mM) mimicking BBB leakage. Conclusions: Early systemic events increasing 131313 permeability may promote entry of cofactors (e. g. K+) into the brain leading to pilocarpine-induced SE. Disturbance of brain homeostasis represents an etiological factor contributing to pilocarpine seizures.

• 出版日期2007-10