Identificador persistente para citar o vincular este elemento: http://hdl.handle.net/10553/128021
Título: The adaptor molecule RIAM integrates signaling events critical for integrin-mediated control of immune function and cancer progression
Autores/as: Patsoukis, N
Bardhan, K
Weaver, JD
Sari, D
Torres Gómez, Álvaro 
Li, LQ
Strauss, L
Lafuente, EM
Boussiotis, VA
Clasificación UNESCO: 32 Ciencias médicas
2412 Inmunología
Fecha de publicación: 2017
Publicación seriada: Science Signaling 
Resumen: Lymphocyte activation requires adhesion to antigen-presenting cells. This is a critical event linking innate and adaptive immunity. Lymphocyte adhesion is accomplished through LFA-1, which must be activated by a process referred to as inside-out integrin signaling.Among the fewsignaling molecules that have been implicated in inside-out integrin activation in hematopoietic cells are the small guanosine triphosphatase (GTPase) Rap1 and its downstream effector Rap1-interacting molecule (RIAM), a multidomain protein that defined the Mig10-RIAM-lamellipodin (MRL) class of adaptor molecules. Through its various domains, RIAM is a critical node of signal integration for activation of T cells, recruits monomeric and polymerized actin to drive actin remodeling and cytoskeletal reorganization, and promotes inside-out integrin signaling in T cells. As a regulator of inside-out integrin activation, RIAMaffectsmultiple functions of innate and adaptive immunity. The effects of RIAM on cytoskeletal reorganization and integrin activation have implications in cell migration and trafficking of cancer cells. Weprovide an overviewof the structure and interactions of RIAM, and we discuss the implications of RIAM functions in innate and adaptive immunity and cancer.
URI: http://hdl.handle.net/10553/128021
ISSN: 1945-0877
DOI: 10.1126/scisignal.aam8298
Fuente: Science Signaling [ISSN 1945-0877], v. 10, n. 493
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