Beneficial effects of EGb761 and vitamin E on haloperidol-induced vacuous chewing movements in rats: Possible involvement of S100B mechanisms

•To compare the effects EGb761 with that of vitamin E for TD and S100B expression in four brain regions.•Both EGb761 and vitamin E significantly prevented the development of TD.•Both EGb761 and vitamin E significantly reversed the increased S100B in all studied brain regions.•Both EGb761 and vitamin...

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Published in:Behavioural brain research 2016-01, Vol.297, p.124-130
Main Authors: An, Hui Mei, Tan, Yun Long, Shi, Jing, Wang, Zhi Ren, Li, Jia, Wang, Yue Chan, Lv, Meng Han, Zhou, Dong Feng, Soares, Jair C., Kosten, Thoams R., Yang, Fu De, Zhang, Xiang Yang
Format: Article
Language:English
Subjects:
Animals
Anti-Dyskinesia Agents - pharmacology
Brain - drug effects
Brain - metabolism
Brain - pathology
Disease Models, Animal
Drug Evaluation, Preclinical
Gingko biloba leaf extract
Haloperidol
Immunohistochemistry
Injections, Intraperitoneal
Male
Mastication - drug effects
Mastication - physiology
Movement Disorders - drug therapy
Movement Disorders - pathology
Movement Disorders - physiopathology
Plant Extracts - pharmacology
Random Allocation
Rats, Sprague-Dawley
S100 Calcium Binding Protein beta Subunit - metabolism
S100B
Tardive dyskinesia
Vitamin E
Vitamin E - pharmacology
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Summary:•To compare the effects EGb761 with that of vitamin E for TD and S100B expression in four brain regions.•Both EGb761 and vitamin E significantly prevented the development of TD.•Both EGb761 and vitamin E significantly reversed the increased S100B in all studied brain regions.•Both EGb761 and vitamin E reduce TD symptoms, possibly via their effects on S100B signaling. Tardive dyskinesia (TD) is a serious side effect induced by the long-term administration of typical antipsychotics. The pathophysiology of TD remains unclear, but experimental evidence suggests that neurodegeneration caused by free radicals may play an important role in TD development. S100B is considered a potential biomarker of structural neural and glial damage. This study investigated S100B expression in TD-related brain regions and assessed the effect of antioxidants Gingko biloba leaf extract (EGb761) and vitamin E (VE) on S100B in TD rats. A total of 32 rats were randomly divided into 4 study groups: saline control (saline), haloperidol alone group (Hal), EGb761-haloperidol (EGb-Hal), and vitamin E-haloperidol (VE-Hal). Rats were treated with haloperidol intraperitoneal injections (2mg/kg/day) each day for 5 weeks. EGb761 (50mg/kg/day) and VE (20mg/kg/day) were then administered during a 5-week withdrawal period. We performed behavioral assessments and immunohistochemically analyzed S100B expression in four TD-related brain regions. Our findings demonstrated that haloperidol administration led to a progressive increase in VCMs and in S100B expression in all four brain regions. Both EGb761 and VE reversed these changes, and there were no group differences between the EGb761 and VE groups. Our results indicated that long-term administration of haloperidol may induce VCMs and increase S100B expression in TD-related brain regions, and S100B may be a significant biomarker related to TD pathophysiology. Moreover, the antioxidant capacity of EGb761 and VE coupled with the possible neuroprotective effects of S100B may account for their success in improving the symptoms of haloperidol-induced TD.
ISSN:0166-4328
1872-7549
DOI:10.1016/j.bbr.2015.10.004