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Target mimicry provides a new mechanism for regulation of microRNA activity

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Fecha
2007-07-22
Autor
Franco Zorrilla, José Manuel
Valli, Adrián
Todesco, Marco
Mateos Moreno, Isabel
Puga, María Isabel
Rubio Somoza, Ignacio
Leyva, Antonio
Weigel, Detlef
García, Juan Antonio
Paz Ares, Javier
Estado
info:eu-repo/semantics/publishedVersion
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Resumen
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MicroRNAs (miRNA) regulate key aspects of development and physiology in animals and plants. These regulatory RNAs act as guides of effector complexes to recognize specific mRNA sequences based on sequence complementarity, resulting in translational repression or site-specific cleavage1,2. In plants, most miRNA targets are cleaved and show almost perfect complementarity with the miRNAs around the cleavage site3,4,5,6,7,8. Here, we examined the non–protein coding gene IPS1 (INDUCED BY PHOSPHATE STARVATION1) from Arabidopsis thaliana. IPS1 contains a motif with sequence complementarity to the phosphate (Pi) starvation–induced miRNA miR-399, but the pairing is interrupted by a mismatched loop at the expected miRNA cleavage site. We show that IPS1 RNA is not cleaved but instead sequesters miR-399. Thus, IPS1 overexpression results in increased accumulation of the miR-399 target PHO2 mRNA and, concomitantly, in reduced shoot Pi content5,6,7,8. Engineering of IPS1 to be cleavable abolishes its inhibitory activity on miR-399. We coin the term 'target mimicry' to define this mechanism of inhibition of miRNA activity. Target mimicry can be generalized beyond the control of Pi homeostasis, as demonstrated using artificial target mimics.
 
URI
https://doi.org/10.1038/ng2079
Target mimicry provides a new mechanism for regulation of microRNA activity
Tipo de Actividad
Artículos en revistas
ISSN
1061-4036
Palabras Clave
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Target mimicry miR-399 IPS1 (INDUCED BY PHOSPHATE STARVATION1) Phosphate (Pi) homeostasis
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Repositorio de la Universidad Pontificia Comillas copyright © 2015  Desarrollado con DSpace Software
Contacto | Sugerencias