dc.description.abstract | Objectives. Blood-brain barrier (BBB) dysfunction is one of the key pathogenic mechanisms in the development of epilepsy. There
is therefore an increasing need to identify BBB biomarkers as these will have prognostic and therapeutic implications. The purpose
of this study was to assess the levels of the BBB permeability markers, glial fibrillary acidic protein (GFAP), neuron-specific
enolase (NSE), S100B, and furin in patients with stable epilepsy compared with the levels in healthy controls. Materials and
Methods. This cross-sectional study included 119 epilepsy patients and 80 healthy controls. Circulating levels of GFAP, NSE,
S100B, and furin were measured and questionnaires regarding epilepsy, use of drugs, and comorbidities were completed by all
participants. Results. GFAP levels were higher in epilepsy patients after adjustment for potential confounders (sex, age, and
BMI) in linear regression (p = 0:042). No significant differences were found in levels of S100B, NSE, or furin. None of the
markers were significantly associated with epilepsy duration, seizure type or severity, or seizures in the preceding six months.
The majority of the patients (79.7%) did not report seizures within the last 6 months. Conclusion. Our main finding is elevated
serum levels of GFAP in epilepsy patients. The results may suggest the presence of astrocyte activation in our patient
population with stable epilepsy. Future prospective studies focusing on the longitudinal relationship between epilepsy debut,
seizures, and time of blood sampling for BBB markers, also within CSF, could provide valuable knowledge including regarding
novel treatment options. The study registration number is 2011/1096, 2018/1437. | en_US |