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Nucleic Acids Research 2005 33(7):2280-2289; doi:10.1093/nar/gki515
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Published online 22 April 2005

© The Author 2005. Published by Oxford University Press. All rights reserved
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Article

Influence of RNA structural stability on the RNA chaperone activity of the Escherichia coli protein StpA

Rupert Grossberger, Oliver Mayer, Christina Waldsich, Katharina Semrad, Sandra Urschitz and Renée Schroeder*

Max F. Perutz Laboratories, University Departments at the Vienna Biocenter, Department of Biochemistry, University of Vienna Dr Bohrgasse 9/5, A-1030 Vienna, Austria

*To whom correspondence should be addressed. Tel: +43 1 4277 54690; Fax: + 43 1 4277 9528; Email: renee.schroeder{at}univie.ac.at

Received February 17, 2005. Revised March 29, 2005. Accepted March 29, 2005.

Proteins with RNA chaperone activity are able to promote folding of RNA molecules by loosening their structure. This RNA unfolding activity is beneficial when resolving misfolded RNA conformations, but could be detrimental to RNAs with low thermodynamic stability. In order to test this idea, we constructed various RNAs with different structural stabilities derived from the thymidylate synthase (td) group I intron and measured the effect of StpA, an Escherichia coli protein with RNA chaperone activity, on their splicing activity in vivo and in vitro. While StpA promotes splicing of the wild-type td intron and of mutants with wild-type-like stability, splicing of mutants with a lower structural stability is reduced in the presence of StpA. In contrast, splicing of an intron mutant, which is not destabilized but which displays a reduced population of correctly folded RNAs, is promoted by StpA. The sensitivity of an RNA towards StpA correlates with its structural stability. By lowering the temperature to 25°C, a temperature at which the structure of these mutants becomes more stable, StpA is again able to stimulate splicing. These observations clearly suggest that the structural stability of an RNA determines whether the RNA chaperone activity of StpA is beneficial to folding.


Present address: Christina Waldsich, Department of Molecular Biophysics and Biochemistry, Yale University, 266 Whitney Avenue, Bass Center, room 325, New Haven, CT 0652 0, USA


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