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Insulin signal transduction through protein kinase cascades
Authors:Avruch  Joseph
Affiliation:(1) Diabetes Unit, Medical Services and the Department of Molecular Biology, Massachusetts General Hospital, USA;(2) Department of Medicine, Harvard Medical School, Boston, MA 02114, USA
Abstract:This review summarizes the evolution of ideas concerning insulin signal transduction, the current information on protein ser/thr kinase cascades as signalling intermediates, and their status as participants in insulin regulation of energy metabolism. Best characterized is the Ras-MAPK pathway, whose input is crucial to cell fate decisions, but relatively dispensable in metabolic regulation. By contrast the effectors downstream of PI-3 kinase, although less well elucidated, include elements indispensable for the insulin regulation of glucose transport, glycogen and cAMP metabolism. Considerable information has accrued on PKB/cAkt, a protein kinase that interacts directly with Ptd Ins 3primeOH phosphorylated lipids, as well as some of the elements further downstream, such as glycogen synthase kinase-3 and the p70 S6 kinase. Finally, some information implicates other erk pathways (e.g. such as the SAPK/JNK pathway) and Nck/cdc42-regulated PAKs (homologs of the yeast Ste 20) as participants in the cellular response to insulin. Thus insulin recruits a broad array of protein (ser/thr) kinases in its target cells to effectuate its characteristic anabolic and anticatabolic programs.
Keywords:insulin action  protein serine/threonine kinase  Ras-raf  MAP kinase  ribosomal S6 protein kinase (RSKs)  phosphatidyl inositol-3 kinase  phrase
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