Insulin alters heterogeneous nuclear ribonucleoprotein K protein binding to DNA and RNA

The interaction of the multimodular heterogeneous nuclear ribo-nucleoprotein (hnRNP) K protein with many of its protein and nucleic acid partners is regulated by extracellular signals. Acting as a docking platform, K protein could link signal-transduction pathways to DNA- and RNA-directed processes such as transcription, mRNA processing, transport, and translation. Treatment of hepatocyte culture with insulin increased K protein tyrosine phosphorylation. Insulin altered K protein interaction with RNA and DNA in vitro. Administration of insulin into mice had similar effects on K protein in liver. Coimmunoprecipitations of RNA with K protein revealed preferential in vivo K protein binding of a subset of transcripts, including the insulin-inducible c-foS mRNA. These results suggest a Bass of insulin pathways that signal nucleic acid-directed processes that involve K protein.