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KMID : 0811720170210060625
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Korean Journal of Physiology & Pharmacology
2017 Volume.21 No. 6 p.625 ~ p.632
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MPTP-induced vulnerability of dopamine neurons in A53T ¥á-synuclein overexpressed mice with the potential involvement of DJ-1 downregulation
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Lee Seong-Mi
Oh Seung-Tack
Jeong Ha-Jin
Pak Sok-Cheon
Park Hi-Joon
Kim Jong-Pil
Cho Hyun-Seok
Jeon Song-Hee
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Abstract
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Familial Parkinson¡¯s disease (PD) has been linked to point mutations and duplication of the ¥á-synuclein (¥á-syn) gene. Mutant ¥á-syn expression increases the vulnerability of neurons to exogenous insults. In this study, we developed a new PD model in the transgenic mice expressing mutant hemizygous (hemi) or homozygous (homo) A53T ¥á-synuclein (¥á-syn Tg) and their wildtype (WT) littermates by treatment with sub-toxic (10 mg/kg, i.p., daily for 5 days) or toxic (30 mg/kg, i.p., daily for 5 days) dose of 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine (MPTP). Tyrosine hydroxylase and Bcl-2 levels were reduced in the ¥á-syn Tg but not WT mice by sub-toxic MPTP injection. In the adhesive removal test, time to remove paper was significantly increased only in the homo ¥á-syn Tg mice. In the challenging beam test, the hemi and homo ¥á-syn Tg mice spent significantly longer time to traverse as compared to that of WT group. In order to find out responsible proteins related with vulnerability of mutant ¥á-syn expressed neurons, DJ-1 and ubiquitin enzyme expressions were examined. In the SN, DJ-1 and ubiquitin conjugating enzyme, UBE2N, levels were significantly decreased in the ¥á-syn Tg mice. Moreover, A53T ¥á-syn overexpression decreased DJ-1 expression in SH-SY5Y cells. These findings suggest that the vulnerability to oxidative injury such as MPTP of A53T ¥á-syn mice can be explained by downregulation of DJ-1.
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KEYWORD
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Apoptosis, DJ-1, MPTP, Parkinson¡¯s disease, Synuclein
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