1. Academic Validation
  2. Dicer-derived microRNAs are utilized by the fragile X mental retardation protein for assembly on target RNAs

Dicer-derived microRNAs are utilized by the fragile X mental retardation protein for assembly on target RNAs

  • J Biomed Biotechnol. 2006;2006(4):64347. doi: 10.1155/JBB/2006/64347.
Isabelle Plante 1 Laetitia Davidovic Dominique L Ouellet Lise-Andrée Gobeil Sandra Tremblay Edouard W Khandjian Patrick Provost
Affiliations

Affiliation

  • 1 Centre de Recherche en Rhumatologie et Immunologie, Centre de Recherche du CHUL-CHUQ, Sainte-Foy, QC, Canada.
Abstract

In mammalian cells, fragile X mental retardation protein (FMRP) has been reported to be part of a MicroRNA (miRNA)-containing effector ribonucleoprotien (RNP) complex believed to mediate translational control of specific mRNAs. Here, using recombinant proteins, we demonstrate that human FMRP can act as a miRNA acceptor protein for the ribonuclease Dicer and facilitate the assembly of miRNAs on specific target RNA sequences. The miRNA assembler property of FMRP was abrogated upon deletion of its single-stranded (ss) RNA binding K-homology domains. The requirement of FMRP for efficient RNA interference (RNAi) in vivo was unveiled by reporter gene silencing assays using various small RNA inducers, which also supports its involvement in an ss small interfering RNA (siRNA)-containing RNP (siRNP) effector complex in mammalian cells. Our results define a possible role for FMRP in RNA silencing and may provide further insight into the molecular defects in patients with the fragile X syndrome.

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