Regulation of Mrna Stability Through a Pentobarbital-Responsive Element
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Akgül, Bünyamin
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Open Access Color
BRONZE
Green Open Access
Yes
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No
Abstract
Pentobarbital, a general anesthetic and non-genotoxic carcinogen, can induce gene expression by activating transcription. In the Drosophila glutathione S-transferase D21 (gstD21) gene, pentobarbital's regulatory influence extends to the level of mRNA turnover. Transcribed from an intronless gene, gstD21 mRNA is intrinsically very labile. But exposure to pentobarbital renders it stabilized beyond what can be attributed to transcriptional activation. We aim here to identify cis-acting element(s) of gstD21 mRNA as contributors to the molecule's pentobarbital-mediated stabilization. In the context of hsp70 5′UTR and the 3′UTR of act5C, gstD21 mRNA, minus its native UTRs, is stable. Maintaining the same context of heterologous UTRs, we can reconstitute using the full-length gstD21 sequence the inherent instability of gstD21 mRNA and its stabilization by pentobarbital. Transgenic flies that express these chimeric gstD21 mRNA exhibit decay intermediates lacking 3′UTR, which are not stabilized by PB treatment. The 3′UTR sequence, when inserted downstream from a reporter transcript, stabilizes it 1.6-fold under PB treatment. The analysis of the decay intermediates suggests a polysome-associated decay pattern. We propose a regulatory model that features a 59-nucleotide pentobarbital-responsive element (PBRE) in the 3′UTR of gstD21 mRNA.
Description
Keywords
Heat shock, mRNA decay, Pentobarbital, Polysome, Polysome, RNA Stability, Response Elements, Animals, Genetically Modified, Heat shock, mRNA decay, Gene Expression Regulation, Animals, Drosophila, RNA, Messenger, Pentobarbital, Glutathione Transferase
Fields of Science
0301 basic medicine, 0303 health sciences, 03 medical and health sciences
Citation
Akgül, B., and Tu, C. P. D. (2007). Regulation of mRNA stability through a pentobarbital-responsive element. Archives of Biochemistry and Biophysics, 459(1), 143-150. doi:10.1016/j.abb.2006.10.026
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OpenCitations Citation Count
3
Volume
459
Issue
1
Start Page
143
End Page
150
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CrossRef : 2
Scopus : 3
PubMed : 1
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3
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3
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1765
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677
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