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A more recent version of this article appeared on November 21, 2001
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M107581200v1
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Papers In Press, published online ahead of print October 3, 2001
J. Biol. Chem, 10.1074/jbc.M107581200
Submitted on August 8, 2001
Revised on October 1, 2001
Accepted on October 3, 2001

The major mRNP protein p50 promotes nucleic acid strand annealing

Maxim A. Skabkin, Valentina M. Evdokimova, Adri A. Thomas, and Lev P. Ovchinnikov

Institute of Protein Research, Russian Acad. Sci., Pushchino, Moscow Region 142290

Corresponding Author: ovchinn{at}vega.protres.ru

p50, a member of the Y-box binding transcription factor family, is tightly associated with eukaryotic mRNAs and is responsible for general translational regulation. Here we show that p50, in addition to its previously described ability to melt mRNA secondary structure, is capable of promoting rapid annealing of complementary nucleic acid strands. p50 accelerates annealing of RNA and DNA duplexes up to 1500-fold within a wide range of salt concentrations and temperatures. Phosphorylation of p50 selectivly inhibits DNA annealing. Moreover, p50 catalyzes strand exchange between double-stranded (ds) and single-stranded (ss) RNAs yielding a product bearing more extended ds structure. Strikingly, p50 displays both RNA-melting and annealing activities in a dose-dependent manner: a relatively low amount of p50 promotes formation of RNA duplexes, whereas an excess of p50 causes unwinding of ds forms. Our results suggest that the alteration of nucleic acid conformation is a basic mechanism of the p50-dependent regulation of gene expression.


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