Artículo
Interactions between RNA-binding proteins and P32 homologues in trypanosomes and human cells
Polledo, Juan Manuel; Cervini Bohm, Gabriela Marta
; Romaniuk, María Albertina
; Cassola, Alejandro Carlos
Fecha de publicación:
02/2016
Editorial:
Springer
Revista:
Current Genetics
ISSN:
0172-8083
e-ISSN:
1432-0983
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
RNA-binding proteins (RBPs) are involved in many aspects of mRNA metabolism such as splicing, nuclear export, translation, silencing, and decay. To cope with these tasks, these proteins use specialized domains such as the RNA recognition motif (RRM), the most abundant and widely spread RNA-binding domain. Although this domain was first described as a dedicated RNA-binding moiety, current evidence indicates these motifs can also engage in direct protein–protein interactions. Here, we discuss recent evidence describing the interaction between the RRM of the trypanosomatid RBP UBP1 and P22, the homolog of the human multifunctional protein P32/C1QBP. Human P32 was also identified while performing a similar interaction screening using both RRMs of TDP-43, an RBP involved in splicing regulation and Amyotrophic Lateral Sclerosis. Furthermore, we show that this interaction is mediated by RRM1. The relevance of this interaction is discussed in the context of recent TDP-43 interactomic approaches that identified P32, and the numerous evidences supporting interactions between P32 and RBPs. Finally, we discuss the vast universe of interactions involving P32, supporting its role as a molecular chaperone regulating the function of its ligands.
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Articulos(IIB-INTECH)
Articulos de INST.DE INVEST.BIOTECNOLOGICAS - INSTITUTO TECNOLOGICO CHASCOMUS
Articulos de INST.DE INVEST.BIOTECNOLOGICAS - INSTITUTO TECNOLOGICO CHASCOMUS
Citación
Polledo, Juan Manuel; Cervini Bohm, Gabriela Marta ; Romaniuk, María Albertina; Cassola, Alejandro Carlos; Interactions between RNA-binding proteins and P32 homologues in trypanosomes and human cells; Springer; Current Genetics; 62; 1; 2-2016; 203-212
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