| Literature DB >> 26923100 |
Xufeng Chen1, Jingjing Xing1, Lei Jiang1, Wenyi Qian2, Yixin Wang2, Hao Sun1, Yu Wang2, Hang Xiao2, Jun Wang3, Jinsong Zhang4.
Abstract
Methamphetamine (METH), an illicit drug, is widely abused in many parts of the world. Mounting evidence shows that METH exposure contributes to neurotoxicity, particularly for the monoaminergic neurons. However, to date, only a few studies have tried to unravel the mechanisms involved in METH-induced non-monoaminergic neural damage. Therefore, in the present study, we tried to explore the mechanisms for METH-induced neural damage in cortical neurons. Our results showed that METH significantly increased intracellular [Ca(2) (+) ]i in Ca(2) (+) -containing solution rather than Ca(2) (+) -free solution. Moreover, METH also upregulated calmodulin (CaM) expression and activated CaM-dependent protein kinase II (CaMKII). Significantly, METH-induced neural damage can be partially retarded by CaM antagonist W7 as well as CaMKII blocker KN93. In addition, L-type Ca(2) (+) channel was also proved to be involved in METH-induced cell damage, as nifedipine, the L-type Ca(2) (+) channel-specific inhibitor, markedly attenuated METH-induced neural damage. Collectively, our results suggest that Ca(2) (+) -CaM-CaMKII is involved in METH-mediated neurotoxicity, and it might suggest a potential target for the development of therapeutic strategies for METH abuse.Entities:
Keywords: CaM; CaMKII; L-type Ca2+ channel; Methamphetamine; neural damage
Mesh:
Substances:
Year: 2016 PMID: 26923100 DOI: 10.1002/jat.3301
Source DB: PubMed Journal: J Appl Toxicol ISSN: 0260-437X Impact factor: 3.446