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The multifunctional protein PEA-15 is involved in the control of apoptosis and cell cycle in astrocytes
Authors:Renault François  Formstecher Etienne  Callebaut Isabelle  Junier Marie-Pierre  Chneiweiss Hervé
Affiliation:INSERM U114, Collège de France, 11 Place Marcelin Berthelot, 75231 Paris Cedex 05, France.
Abstract:
PEA-15 is a small protein (15 kDa) that was first identified as an abundant phosphoprotein in brain astrocytes [Araujo et al., J Biol Chem 1993;268(8):5911-20], and subsequently shown to be widely expressed in different tissues and highly conserved among mammals [Estelles et al., J Biol Chem 1996;271(25):14800-6; Danziger et al., J Neurochem 1995;64(3):1016-25]. It is composed of a N-terminal death effector domain and a C-terminal tail of irregular structure. PEA-15 is regulated by multiple calcium-dependent phosphorylation pathways that account for its different forms: a non-phosphorylated form in equilibrium with a mono and a biphosphorylated variety. This already suggested that PEA-15 may play a major role in signal integration. Accordingly, it has been demonstrated to modulate signaling pathways that control apoptosis and cell proliferation. In particular, PEA-15 diverts astrocytes from TNFalpha-triggered apoptosis and regulates the actions of the ERK MAP kinase cascade by binding to ERK and altering its subcellular localization. The three-dimensional structure of PEA-15 has been modelized and recently determined using NMR spectroscopy, and may help to understand the various functions played by the protein through its molecular interactions.
Keywords:DED, death effector domain   PKC, protein kinase C   ERK MAP kinase, extracellular regulated kinase mitogen-associated protein kinase   NMR, nuclear magnetic resonance   TNFalpha, tumor necrosis factor alpha   CaMKII, calcium-calmodulin-dependent kinase type II   FADD, Fas-associated death domain   PLD1/PLD2, phospholipase D1 and D2
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