Preischemic hyperglycemia is known to aggravate brain damage caused by transient forebrain ischemia. Because heat shock proteins (HSPs) 72 have been proposed to play a protective role against ischemic neuronal injury, we studied the HSP 72 mRNA expression and protein synthesis in gerbils subjected to 10 min bilateral carotid occlusion under normoglycemic, hyperglycemic and fasting conditions. HSP 72 mRNA expression and HSP 72 synthesis were studied using in situ hybridization and immunostaining, respectively. After 8 h of blood recirculation, HSP 72 mRNAs were expressed in all the hippocampal subfields of the three different groups, with higher expression in the hyperglycemic gerbils. After 48 h of reperfusion, HSP 72 mRNAs had almost completely disappeared in the hyper- and normoglycemic groups, and were more strongly expressed in the CA 1 neurons of the fasted group. At this time, fasted gerbils exhibited intense HSP 72 immunoreactivity in the CA 1, whereas an absence of immunoreactivity was observed in that area in the other groups. Finally, ischemia was also associated with marked astrocytic activation, as evidenced by GFAP immunostaining. Overall results indicate that preischemic differences in blood glucose supply to the brain are related to HSP 72 mRNA expression (in terms of duration) and to HSP 72 protein induction (in terms of intensity) in the vulnerable CA 1 neurons of the hippocampus. Ability of CA 1 neurons to synthesize HSP 72 proteins was associated with higher neuronal survival in the fasted group after 48 h of reflow, suggesting a protective role of HSP 72, even though evaluation of neuronal damage at 7 days indicated that neuronal death was mainly delayed in the time.