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Control of PKA stability and signalling by the RING ligase praja2.

Nat Cell Biol.. 2011-04;  13(4):412-22
Lignitto L, Carlucci A, Sepe M, Stefan E, Cuomo O, NisticÒ R, Scorziello A, Savoia C, Garbi C, Annunziato L, Feliciello A.
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摘要

Activation of G-protein-coupled receptors (GPCRs) mobilizes compartmentalized pulses of cyclic AMP. The main cellular effector of cAMP is protein kinase A (PKA), which is assembled as an inactive holoenzyme consisting of two regulatory (R) and two catalytic (PKAc) subunits. cAMP binding to R subunits dissociates the holoenzyme and releases the catalytic moiety, which phosphorylates a wide array of cellular proteins. Reassociation of PKAc and R components terminates the signal. Here we report that the RING ligase praja2 controls the stability of mammalian R subunits. Praja2 forms a stable complex with, and is phosphorylated by, PKA. Rising cAMP levels promote praja2-mediated ubiquitylation and subsequent proteol... More

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