Regulation of Connexin-43-Mediated Growth Inhibition by a Phosphorylatable Amino-Acid is Independent of Gap Junction-Forming Ability |
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| Authors: | Xitong Dang Madhumathy Jeyaraman Elissavet Kardami |
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| Institution: | (1) Departments of Human Anatomy and Cell Sciences and Physiology, University of Manitoba, Winnipeg, R2H 2A6, Canada;(2) Institute of Cardiovascular Sciences, St. Boniface Research Centre, 351 Tache Ave, Winnipeg, MB, R2H 2A6, Canada |
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| Abstract: | The ability of the gap junction phosphoprotein connexin-43 (Cx43) to inhibit DNA synthesis in primary cardiomyocytes is regulated by serine (S) 262, a protein kinase C phosphorylation site that also affects metabolic coupling. We have now examined if the S262-regulated growth suppression is operating in transformed cells and if so whether it depends on gap junction channel forming ability. Serine 262 became phosphorylated in response to protein kinase C stimulation in HEK293 cells transiently expressing either Cx43 or the non-channel-forming carboxy-terminal tail of Cx43 (Cx43CT). Expression of either wild type Cx43 or Cx43CT inhibited DNA synthesis, as did their mutated versions simulating lack of phosphorylation by carrying an S262-to-alanine substitution. The ability to inhibit DNA synthesis was eliminated when expressing mutated versions of either Cx43 or Cx43CT simulating constitutive phosphorylation by carrying an S262-to-aspartate substitution. We conclude that S262 phosphorylation cancels growth inhibition by Cx43 independently of channel-forming ability. |
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| Keywords: | growth regulation connexins phosphorylation structure-function protein kinase C |
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