Artículo
Different cAMP sources are critically involved in G protein-coupled receptor CRHR1 signaling
Inda, María Carolina
; Dos Santos Claro, Paula Ayelen
; Bonfiglio, Juan José
; Senin, Sergio Ariel
; Maccarrone, Giuseppina; Turck, Christoph W.; Silberstein Cuña, Susana Iris
Fecha de publicación:
07/2016
Editorial:
Rockefeller University Press
Revista:
Journal of Cell Biology
ISSN:
0021-9525
e-ISSN:
1540-8140
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
Corticotropin-releasing hormone receptor 1 (CRHR1) activates G protein-dependent and internalization-dependent signaling mechanisms. Here, we report that the cyclic AMP (cAMP) response of CRHR1 in physiologically relevant scenarios engages separate cAMP sources, involving the atypical soluble adenylyl cyclase (sAC) in addition to transmembrane adenylyl cyclases (tmACs). cAMP produced by tmACs and sAC is required for the acute phase of extracellular signal regulated kinase 1/2 activation triggered by CRH-stimulated CRHR1, but only sAC activity is essential for the sustained internalization-dependent phase. Thus, different cAMP sources are involved in different signaling mechanisms. Examination of the cAMP response revealed that CRH-activated CRHR1 generates cAMP after endocytosis. Characterizing CRHR1 signaling uncovered a specific link between CRH-activated CRHR1, sAC, and endosome-based signaling. We provide evidence of sAC being involved in an endocytosis-dependent cAMP response, strengthening the emerging model of GPCR signaling in which the cAMP response does not occur exclusively at the plasma membrane and introducing the notion of sAC as an alternative source of cAMP.
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Articulos(IBIOBA - MPSP)
Articulos de INST. D/INV.EN BIOMED.DE BS AS-CONICET-INST. PARTNER SOCIEDAD MAX PLANCK
Articulos de INST. D/INV.EN BIOMED.DE BS AS-CONICET-INST. PARTNER SOCIEDAD MAX PLANCK
Citación
Inda, María Carolina; Dos Santos Claro, Paula Ayelen; Bonfiglio, Juan José; Senin, Sergio Ariel; Maccarrone, Giuseppina; et al.; Different cAMP sources are critically involved in G protein-coupled receptor CRHR1 signaling; Rockefeller University Press; Journal of Cell Biology; 214; 2; 7-2016; 181-195
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