Literature DB >> 9735368

The K box, a conserved 3' UTR sequence motif, negatively regulates accumulation of enhancer of split complex transcripts.

E C Lai1, C Burks, J W Posakony.   

Abstract

Cell-cell interactions mediated by the Notch receptor play an essential role in the development of the Drosophila adult peripheral nervous system (PNS). Transcriptional activation of multiple genes of the Enhancer of split Complex [E(spl)-C] is a key intracellular response to Notch receptor activity. Here we report that most E(spl)-C genes contain a novel sequence motif, the K box (TGTGAT), in their 3' untranslated regions (3' UTRs). We present three lines of evidence that demonstrate the importance of this element in the post-transcriptional regulation of E(spl)-C genes. First, K box sequences are specifically conserved in the orthologs of two structurally distinct E(spl)-C genes (m4 and m8) from a distantly related Drosophila species. Second, the wild-type m8 3' UTR strongly reduces accumulation of heterologous transcripts in vivo, an activity that requires its K box sequences. Finally, m8 genomic DNA transgenes lacking these motifs cause mild gain-of-function PNS defects and can partially phenocopy the genetic interaction of E(spl)D with Notchspl. Although E(spl)-C genes are expressed in temporally and spatially specific patterns, we find that K box-mediated regulation is ubiquitous, implying that other targets of this activity may exist. In support of this, we present sequence analyses that implicate genes of the iroquois Complex (Iro-C) and engrailed as additional targets of K box-mediated regulation.

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Year:  1998        PMID: 9735368     DOI: 10.1242/dev.125.20.4077

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  74 in total

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Journal:  Development       Date:  2012-06-28       Impact factor: 6.868

4.  Evolution of a genomic regulatory domain: the role of gene co-option and gene duplication in the Enhancer of split complex.

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Journal:  Genome Res       Date:  2010-05-10       Impact factor: 9.043

Review 5.  MicroRNAs in opioid pharmacology.

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6.  Pervasive regulation of Drosophila Notch target genes by GY-box-, Brd-box-, and K-box-class microRNAs.

Authors:  Eric C Lai; Bergin Tam; Gerald M Rubin
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7.  Functional screening identifies miR-315 as a potent activator of Wingless signaling.

Authors:  Serena J Silver; Joshua W Hagen; Katsutomo Okamura; Norbert Perrimon; Eric C Lai
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8.  Reliable prediction of regulator targets using 12 Drosophila genomes.

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9.  The mir-279/996 cluster represses receptor tyrosine kinase signaling to determine cell fates in the Drosophila eye.

Authors:  Hong Duan; Luis F de Navas; Fuqu Hu; Kailiang Sun; Yannis E Mavromatakis; Kayla Viets; Cyrus Zhou; Joshua Kavaler; Robert J Johnston; Andrew Tomlinson; Eric C Lai
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10.  Systematic discovery and characterization of fly microRNAs using 12 Drosophila genomes.

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