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http://dx.doi.org/10.5012/bkcs.2013.34.7.2063

Phosphorylation-Dependent Mobility Shift of Proteins on SDS-PAGE is Due to Decreased Binding of SDS  

Lee, Chang-Ro (Department of Biological Sciences and Institute of Microbiology, Seoul National University)
Park, Young-Ha (Department of Biological Sciences and Institute of Microbiology, Seoul National University)
Kim, Yeon-Ran (Department of Biological Sciences and Institute of Microbiology, Seoul National University)
Peterkofsky, Alan (Laboratory of Cell Biology, National Heart, Lung, and Blood Institute, National Institutes of Health)
Seok, Yeong-Jae (Department of Biological Sciences and Institute of Microbiology, Seoul National University)
Publication Information
Abstract
While many eukaryotic and some prokaryotic proteins show a phosphorylation-dependent mobility shift (PDMS) on SDS-PAGE, the molecular mechanism for this phenomenon had not been elucidated. We have recently shown that the distribution of negatively charged amino acids around the phosphorylation site is important for the PDMS of some proteins. Here, we show that replacement of the phosphorylation site with a negatively charged amino acid results in a similar degree of the mobility shift of a protein as phosphorylation, indicating that the PDMS is due to the introduction of a negative charge by phosphorylation. Compared with a protein showing no shift, one showing a retarded mobility on SDS-PAGE had a decreased capacity for SDS binding. The elucidation of the consensus sequence (${\Theta}X_{1-3}{\Theta}X_{1-3}{\Theta}$, where ${\Theta}$ corresponds to an acidic function) for a PDMS suggests a general strategy for mutagenizing a phosphorylatable protein resulting in a PDMS.
Keywords
Electrophoretic mobility shift; Protein phosphorylation; SDS-PAGE; Signal transduction;
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