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| Indexado |
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| DOI | 10.1007/S11302-022-09913-Y | ||||
| Año | 2022 | ||||
| Tipo | revisión |
Citas Totales
Autores Afiliación Chile
Instituciones Chile
% Participación
Internacional
Autores
Afiliación Extranjera
Instituciones
Extranjeras
Transactivation of receptor tyrosine kinases (RTK) is a crosstalk mechanism exhibited by G-protein–coupled receptors (GPCR) to activate signaling pathways classically associated with growth factors. The discovery of RTK transactivation was a breakthrough in signal transduction that contributed to developing current concepts in intracellular signaling. RTK transactivation links GPCR signaling to important cellular processes, such as cell proliferation and differentiation, and explains the functional diversity of these receptors. Purinergic (P2Y and adenosine) receptors belong to class A of GPCR; in the present work, we systematically review the experimental evidence showing that purinergic receptors have the ability to transactivate RTK in multiple tissues and physiopathological conditions resulting in the modulation of cellular physiology. Of particular relevance, the crosstalk between purinergic receptors and epidermal growth factor receptor is a redundant pathway that participates in multiple pathophysiological processes. Specific and detailed knowledge of purinergic receptor-regulated pathways advances our understanding of the complexity of GPCR signal transduction and opens the way for pharmacologic intervention in the pathological context.
| Ord. | Autor | Género | Institución - País |
|---|---|---|---|
| 1 | Vazquez-Cuevas, Francisco G. | Hombre |
Instituto de Neurobiología, UNAM - México
Univ Nacl Autonoma Mexico - México |
| 2 | Reyna-Jeldes, Mauricio | Hombre |
Universidad Católica del Norte - Chile
Núcleo Milenio para el Estudio del Dolor - Chile |
| 3 | Velazquez-Miranda, Erandi | - |
Instituto de Neurobiología, UNAM - México
Univ Nacl Autonoma Mexico - México |
| 4 | CODDOU-ALVAREZ, CLAUDIO EDUARDO | Hombre |
Universidad Católica del Norte - Chile
Núcleo Milenio para el Estudio del Dolor - Chile |
| Fuente |
|---|
| Direccion General de Asuntos del Personal Academico, Universidad Nacional Autonoma de Mexico |
| VRIDT |
| Ministerio de Ciencia, Tecnología, Conocimiento e Innovación |
| Millennium Nucleus for the Study of Pain (MiNuSPain) |
| Nivel Básico, Aplicado y Clínico |
| Millennium Scientific Initiative of the Ministry of Science, Technology, Knowledge and Innovation, Chile |
| Direccion General de Asuntos del Personal Academico (DGAPA-UNAM) |
| Nucleo para el Estudio del Cancer a Nivel Basico, Aplicado y Clinico, VRIDT UCN |
| Agradecimiento |
|---|
| This work was supported by Dirección General de Asuntos del Personal Académico (DGAPA-UNAM) (IN202620 and IN205223 to FGVC), Núcleo para el Estudio del Cáncer a Nivel Básico, Aplicado y Clínico, VRIDT UCN 20210401007 (C.C.), and by the Millennium Nucleus for the Study of Pain (MiNuSPain). MiNuSPain is supported by the Millennium Scientific Initiative NCN19_038 of the Ministry of Science, Technology, Knowledge and Innovation, Chile (C.C.). |
| This work was supported by Direccion General de Asuntos del Personal Academico (DGAPA-UNAM) (IN202620 and IN205223 to FGVC), Nucleo para el Estudio del Cancer a Nivel Basico, Aplicado y Clinico, VRIDT UCN 20210401007 (C.C.), and by the Millennium Nucleus for the Study of Pain (MiNuSPain). MiNuSPain is supported by the Millennium Scientific Initiative NCN19_038 of the Ministry of Science, Technology, Knowledge and Innovation, Chile (C.C.). |