Affiliations: Cerebrovascular Research Center, Department of
Neurological Surgery Cleveland Clinic Foundation, Cleveland, OH 44195,
USA | Cerebrovascular Research Center, Department of Cell
Biology, Cleveland Clinic Foundation, Cleveland, OH 44195, USA
Abstract: Purpose: Occurrence of brain damage is frequently associated with
abnormal blood-brain barrier (BBB) function. Two brain-specific proteins,
S100β and neuron-specific enolase (NSE) are released systemically in a
variety of neurological diseases, but S100β levels sometimes rise in the
absence of neuronal damage, suggesting that S100β is a marker of BBB
rather than neuronal damage. Methods: We measured both proteins in the serum of patients
undergoing iatrogenic BBB disruption with intrarterial mannitol, followed by
chemotherapy. Results: Serum S100β increased significantly after mannitol
infusion (p<0.05) while NSE did not. Furthermore, in a model of
intracerebral hemorrhage, S100β increases in CSF did not lead to serum
changes at a time when the BBB was intact. Modeling of S100β release from
the CNS suggested that low (<0.34 ng/ml) serum levels of S100β are
consistent with BBB opening without CNS damage, while larger increases imply
synthesis and release from presumable damaged glia. Conclusions: Thus, S100β in serum is an early marker of BBB
openings that may precede neuronal damage and may influence therapeutic
strategies. Secondary, massive elevations in S100β are indicators of
prior brain damage and bear clinical significance as predictors of poor outcome
or diagnostic means to differentiate extensive damage from minor, transient
impairment.
