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Journal of Zhejiang University-SCIENCE B (Biomedicine & Biotechnology)  2011, Vol. 12 Issue (12): 951-960    DOI: 10.1631/jzus.B1100121
Biochemistry     
Effect of microcystin-LR on protein phosphatase 2A and its function in human amniotic epithelial cells
Jing Liang, Tan Li, Ya-li Zhang, Zong-lou Guo, Li-hong Xu
Department of Biochemistry and Genetics, School of Medicine, Zhejiang University, Hangzhou 310058, China, Department of Biosystem Engineering, College of Biosystem Engineering and Food Science, Zhejiang University, Hangzhou 310058, China
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Abstract  Due to their toxicity, the increased distribution of microcystins (MCs) has become an important worldwide problem. MCs have been recognized as inhibitors of protein phosphatase 2A (PP2A) through their binding to the PP2A catalytic subunit. However, the exact mechanism of MC toxicity has not been elucidated, especially concerning the cellular response and its autoregulation. To further dissect the role of PP2A in MC-induced toxicity, the present study was undertaken to determine the response of PP2A in human amniotic epithelial (FL) cells treated with microcystin-LR (MCLR), one of the MC congeners. The results show that a low-dose treatment of MCLR in FL cells for 6 h induced an increase in PP2A activity, and a high-dose treatment of MCLR for 24 h decreased the activity of PP2A, as expected. The increased mRNA and protein levels of the PP2A C subunit may explain the increased activity of PP2A. Furthermore, MCLR altered microtubule post-translational modifications through PP2A. These results further clarify the underlying mechanism how MCLR affects PP2A and may be helpful for elucidating the complex toxicity of MCLR.

Key wordsMicrocystin-LR      Protein phosphatase 2A      Phosphatase activity      Hormesis      Tubulin      B55α     
Received: 13 April 2011      Published: 30 November 2011
CLC:  Q26  
Cite this article:

Jing Liang, Tan Li, Ya-li Zhang, Zong-lou Guo, Li-hong Xu. Effect of microcystin-LR on protein phosphatase 2A and its function in human amniotic epithelial cells. Journal of Zhejiang University-SCIENCE B (Biomedicine & Biotechnology), 2011, 12(12): 951-960.

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http://www.zjujournals.com/xueshu/zjus-b/10.1631/jzus.B1100121     OR     http://www.zjujournals.com/xueshu/zjus-b/Y2011/V12/I12/951

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