Anti-Rex Aptamers as Mimics of the Rex-Binding Element

Author:

Baskerville Scott1,Zapp Maria2,Ellington Andrew D.3

Affiliation:

1. Department of Biology1and

2. Department of Molecular Genetics and Microbiology, University of Massachusetts Cancer Center, Worchester, Massachusetts2

3. Department of Chemistry,3 Indiana University at Bloomington, Bloomington, Indiana, and

Abstract

ABSTRACT RNA molecules that bind tightly and specifically to a Rex fusion protein have been isolated from a conformationally constrained pool of random sequence RNAs. The anti-Rex aptamers effectively mimic several features of the wild-type Rex-binding element (XBE). The highest-affinity aptamers effectively compete with the wild-type XBE for binding to the RNA-binding domain of Rex, an arginine-rich motif (ARM), but do not bind to the functionally analogous Rev protein or its ARM. However, characteristic sequence and structural motifs found in some of the anti-Rex aptamers may provide insights into how the Rex protein can interact with other viral RNAs, such as the Rev-responsive element. The anti-Rex aptamers can functionally substitute for the XBE in vivo, a result which supports a previously proposed model for mRNA transport in which the viral genome serves as a platform for assembling a nucleoprotein complex that can co-opt the cellular transport apparatus. Overall, these studies suggest that anti-Rex aptamers may serve as RNA decoys of the Rex protein.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

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