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| DOI | 10.1091/MBC.E10-02-0167 | ||
| Año | 2010 | ||
| Tipo | artículo de investigación |
Citas Totales
Autores Afiliación Chile
Instituciones Chile
% Participación
Internacional
Autores
Afiliación Extranjera
Instituciones
Extranjeras
Endocytosis modulates EGFR function by compartmentalizing and attenuating or enhancing its ligand-induced signaling. Here we show that it can also control the cell surface versus intracellular distribution of empty/inactive EGFR. Our previous observation that PKA inhibitors induce EGFR internalization prompted us to test phosphatidic acid (PA) generated by phospholipase D (PLD) as an endogenous down-regulator of PKA activity, which activates rolipram-sensitive type 4 phosphodiesterases (PDE4) that degrade cAMP. We found that inhibition of PA hydrolysis by propranolol, in the absence of ligand, provokes internalization of inactive (neither tyrosine-phosphorylated nor ubiquitinated) EGFR, accompanied by a transient increase in PA levels and PDE4s activity. This EGFR internalization is mimicked by PA micelles and is strongly counteracted by PLD2 silencing, rolipram or forskolin treatment, and PKA overexpression. Accelerated EGFR endocytosis seems to be mediated by clathrin-dependent and -independent pathways, leading to receptor accumulation in juxtanuclear recycling endosomes, also due to a decreased recycling. Internalized EGFR can remain intracellular without degradation for several hours or return rapidly to the cell surface upon discontinuation of the stimulus. This novel regulatory mechanism of EGFR, also novel function of signaling PA, can transmodulate receptor accessibility in response to heterologous stimuli.
| Ord. | Autor | Género | Institución - País |
|---|---|---|---|
| 1 | Norambuena, Andres | Hombre | |
| 2 | METZ-BAER, CLAUDIA ANDREA | Mujer | |
| 3 | Jung, Juan E. | Hombre | |
| 4 | SILVA-ALDANA, ANTONIA FRANCISCA | Mujer | |
| 5 | OTERO-ACUNA, MARIA CAROLINA | Mujer | |
| 6 | CANCINO-NUNEZ, JOSE IGNACIO | Hombre | |
| 7 | Retamal, Claudio | Hombre | |
| 8 | Valenzuela, Juan C. | Hombre | |
| 9 | SOZA-GAJARDO, ANDREA MORENA | Mujer | |
| 10 | GONZALEZ-RUIZ, AIXA | Hombre |
Pontificia Universidad Católica de Chile - Chile
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| Fuente |
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| FONDECYT |
| Pontificia Universidad Católica de Chile |
| Fondo Nacional de Areas Prioritarias (FONDAP) |
| Comision de Investigacion Cientifica y Tecnologica (CONICYT) |
| Ministerio de Planificacion y Cooperacion de Chile |
| Agradecimiento |
|---|
| We thank Drs. Maria Rosa Bono, Tulio Nunez, Michael Frohman and Manuela Zaccolo for their kind gift of reagents. This work received financial support from Fondo Nacional de Areas Prioritarias (FONDAP) Grant 13980001, Programa de Financiamiento Basal para Centros de Excelencia Grant PFB12/2007 from the Comision de Investigacion Cientifica y Tecnologica (CONICYT), and FONDECYT Grant 1100747, doctoral fellowships to A.N. and A.S. from the Pontificia Universidad Catolica de Chile, and a postdoctoral fellowship to C.O. from CONICYT. The Millennium Institute for Fundamental and Applied Biology (MIFAB) is financed in part by the Ministerio de Planificacion y Cooperacion de Chile. |