Glutamate Excitotoxicity Is Involved in Cell Death Caused by Tributyltin in Cultured Rat Cortical Neurons

doi:10.1093/toxsci/kfj007

ToxSci Advance Access originally published online on October 5, 2005
Toxicological Sciences 2006 89(1):235-242; doi:10.1093/toxsci/kfj007

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Glutamate Excitotoxicity Is Involved in Cell Death Caused by Tributyltin in Cultured Rat Cortical Neurons

Yusuke Nakatsu^*, Yaichiro Kotake^*^,^,1, Kazuya Komasaka^*, Hiroko Hakozaki^*, Ryota Taguchi, Toshiaki Kume, Akinori Akaike and Shigeru Ohta^*

^* Graduate School of Biomedical Sciences, Hiroshima University, 1–2–3, Kasumi, Minami-ku, Hiroshima, 734-8551, Japan; Center for Quantum Life Sciences, Hiroshima University, 1–2–3, Kasumi, Minami-ku, Hiroshima, 734-8551, Japan; Graduate School of Pharmaceutical Sciences, Kyoto University, 46–29, Yoshida-Shimoadachi-cho, Sakyo-ku, Kyoto, 606-8501, Japan

Received August 9, 2005; accepted September 25, 2005

Tributyltin, an endocrine-disrupting chemical, has been usedas a heat stabilizer, agricultural pesticide, and componentof antifouling paints. In this study, the neurotoxicity of tributyltinwas investigated in cultured rat cortical neurons. Tributyltincaused marked time- and dose-dependent increases in the numberof trypan blue–stained cells. Measurement of extracellularglutamate concentration showed that glutamate release was inducedby tributyltin. Application of the glutamate receptor antagonistsMK-801 and CNQX decreased the neurotoxicity. These results suggestthat released glutamate and glutamate receptors are involvedin tributyltin toxicity. Next, we examined whether various factors,believed to be involved in glutamate excitotoxicity also influencetributyltin toxicity. Cell death induced by tributyltin wasfound to be reduced by ${alpha}$ -tocopherol (a membrane-permeable antioxidant),SB202190 (a p38 mitogen-activated protein kinase inhibitor),and U-0126 (an extracellular signal-regulated protein kinasekinase inhibitor). MK-801 and CNQX decreased the phosphorylationof ERK, but not that of p38. A caspase-3 inhibitor had no effecton tributyltin toxicity, and tributyltin did not change thenuclear morphology. These results suggest that the glutamateexcitotoxicity caused by tributyltin is unrelated to apoptosis.In conclusion, we demonstrated that tributyltin induced glutamaterelease and subsequent activation of glutamate receptors, leadingto neuronal death. We propose two independent neuronal deathpathways by tributyltin; one is glutamate receptor–dependentcell death via ERK phosphorylation, and the other may be glutamatereceptor–independent cell death via p38 activation.

Key Words: tributyltin-glutamate release-NMDA receptors; reactive oxygen species; mitogen-activated protein kinase; caspase.

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This article has been cited by other articles:

Y. Nakatsu, Y. Kotake, and S. Ohta
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