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Merck
  • Identification of the proteins related to SET-mediated hepatic cytotoxicity of trichloroethylene by proteomic analysis.

Identification of the proteins related to SET-mediated hepatic cytotoxicity of trichloroethylene by proteomic analysis.

Toxicology letters (2014-03-19)
Xiaohu Ren, Xifei Yang, Wen-Xu Hong, Peiwu Huang, Yong Wang, Wei Liu, Jinbo Ye, Haiyan Huang, Xinfeng Huang, Liming Shen, Linqing Yang, Zhixiong Zhuang, Jianjun Liu
摘要

Trichloroethylene (TCE) is an effective solvent for a variety of organic materials. Since the wide use of TCE as industrial degreasing of metals, adhesive paint and polyvinyl chloride production, TCE has turned into an environmental and occupational toxicant. Exposure to TCE could cause severe hepatotoxicity; however, the toxic mechanisms of TCE remain poorly understood. Recently, we reported that SET protein mediated TCE-induced cytotoxicity in L-02 cells. Here, we further identified the proteins related to SET-mediated hepatic cytotoxicity of TCE using the techniques of DIGE (differential gel electrophoresis) and MALDI-TOF-MS/MS. Among the 20 differential proteins identified, 8 were found to be modulated by SET in TCE-induced cytotoxicity and three of them (cofilin-1, peroxiredoxin-2 and S100-A11) were validated by Western-blot analysis. The functional analysis revealed that most of the identified SET-modulated proteins are apoptosis-associated proteins. These data indicated that these proteins may be involved in SET-mediated hepatic cytotoxicity of TCE in L-02 cells.

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三氯乙烯, ACS reagent, ≥99.5%
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三氯乙烯, analytical standard, stabilized with 30 – 50 ppm Diisopropylamine
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三氯乙烯 溶液, certified reference material, 5000 μg/mL in methanol
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