ELAV mediates 3′ UTR extension in the Drosophila nervous system (original) (raw)

1. Sandra B. Lemke and
2. Michael Levine1
3. Division of Genetics, Genomics, and Development, Department of Molecular and Cell Biology, Center for Integrative Genomics, University of California at Berkeley, Berkeley, California 94720, USA

Abstract

Post-transcriptional gene regulation is prevalent in the nervous system, where multiple tiers of regulatory complexity contribute to the development and function of highly specialized cell types. Whole-genome studies in Drosophila have identified several hundred genes containing long 3′ extensions in neural tissues. We show that ELAV (embryonic-lethal abnormal visual system) is a key mediator of these neural-specific extensions. Misexpression of ELAV results in the ectopic synthesis of long messenger RNAs (mRNAs) in transgenic embryos. RNA immunoprecipitation assays suggest that ELAV directly binds the proximal polyadenylation signals of many target mRNAs. Finally, ELAV is sufficient to suppress 3′ end formation at a strong polyadenylation signal when tethered to a synthetic RNA. We propose that this mechanism for coordinating 3′ UTR extension may be generally used in a variety of cellular processes.

• ELAV
• alternative polyadenylation
• 3′ UTR
• nervous system
• extension
• post-transcriptional regulation

Footnotes

• ↵1 Corresponding author
  E-mail mlevine{at}berkeley.edu

• Supplemental material is available for this article.

• Article published online ahead of print. Article and publication date are online at http://www.genesdev.org/cgi/doi/10.1101/gad.199653.112.

• Received June 27, 2012.

• Accepted August 27, 2012.

• Copyright © 2012 by Cold Spring Harbor Laboratory Press

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