1-42 beta-Amyloid peptide requires PDK1/nPKC/Rac 1 pathway to induce neuronal death

Manterola, L.; Hernando Rodríguez, M.; Ruiz Núñez, Asier; Apraiz, A.; Arrizabalaga Uriarte, Oskar; Vellon, L.; Alberdi Alfonso, Elena María; Cavaliere, Fabio; Lacerda, Hadriano M.; Jimenez, S.; Parada, L. A.; Matute Almau, Carlos José; Zugaza Gurruchaga, José Luis

Ikusi/Ireki

tp2012147a.pdf (1.322Mb)

Data

2013-01

Egilea

Manterola, L.

Hernando Rodríguez, M.

Ruiz Núñez, Asier

Apraiz, A.

Arrizabalaga Uriarte, Oskar

Vellon, L.

Alberdi Alfonso, Elena María

Cavaliere, Fabio

Lacerda, Hadriano M.

Jimenez, S.

Parada, L. A.

Matute Almau, Carlos José

Zugaza Gurruchaga, José Luis

Metadata

Itemaren erregistro osoa erakusten du

Estadisticas en RECOLECTA
(LA Referencia)

Translational Psychiatry 3 : (2013) // e219

URI

http://hdl.handle.net/10810/11340

Laburpena

1-42 beta-Amyloid (A beta(1-42)) peptide is a key molecule involved in the development of Alzheimer's disease. Some of its effects are manifested at the neuronal morphological level. These morphological changes involve loss of neurites due to cytoskeleton alterations. However, the mechanism of A beta(1-42) peptide activation of the neurodegenerative program is still poorly understood. Here, A beta(1-42) peptide-induced transduction of cellular death signals through the phosphatidylinositol 3-kinase (PI3K)/phosphoinositol- dependent kinase (PDK)/novel protein kinase C (nPKC)/Rac 1 axis is described. Furthermore, pharmacological inhibition of PDK1 and nPKC activities blocks Rac 1 activation and neuronal cell death. Our results provide insights into an unsuspected connection between PDK1, nPKCs and Rac 1 in the same signal-transduction pathway and points out nPKCs and Rac 1 as potential therapeutic targets to block the toxic effects of A beta(1-42) peptide in neurons.