RNA-binding Ability of PIPPin Requires the Entire Protein

Overview

Journal J Cell Mol Med

Specialties Cell Biology
Molecular Biology

Date 2003 May 28

PMID 12767259

Citations 3

Authors

Lavinia Raimondi

Matilde DAsaro

Patrizia Proia

Tommaso Nastasi

Italia Di Liegro

Affiliations

Soon will be listed here.

Abstract

Post-transcriptional fate of eukaryotic mRNAs depends on association with different classes of RNA-binding proteins (RBPs). Among these proteins, the cold-shock domain (CSD)-containing proteins, also called Y-box proteins, play a key role in controlling the recruitment of mRNA to the translational machinery, in response to environmental cues, both in development and in differentiated cells. We recently cloned a rat cDNA encoding a new CSD-protein that we called PIPPin. This protein also contains two putative double-stranded RNA-binding motifs (PIP(1) and PIP(2)) flanking the central CSD, and is able to bind mRNAs encoding H1 degrees and H3.3 histone variants. In order to clarify the role of each domain in the RNA-binding activity of PIPPin, we constructed a number of different recombinant vectors, encoding different regions of the protein. Here we report that only recombinant proteins that contain all the putative PIPPin domains show RNA-binding ability.

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