Dual sex-specific functions of<i>Drosophila</i>Upstream of N-ras in the control of X chromosome dosage compensation

Patalano, Solenn; Mihailovich, Marija; Belacortu, Yaiza; Paricio, Nuria; Gebauer, Fátima

doi:10.1242/dev.027656

Cited by 24 publications

(29 citation statements)

References 44 publications

(56 reference statements)

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“…Sequencing allows the unbiased identification of targets, including non-annotated transcripts and noncoding RNAs. Because UNR binds to the nuclear noncoding RNAs roX1 and roX2 (Patalano et al 2009), in order to identify coding and noncoding poly(A) + transcripts bound by UNR independently of their subcellular distribution, we used total male and female adult extracts for RIP-seq. A RIP experiment including a duplicate with anti-UNR antibodies and one IgG control was performed per sex, and the RNA isolated from the pellet was sequenced (Fig.…”

Section: Identification Of Unr Targetsmentioning

confidence: 99%

“…X-chromosome dosage compensation is the process that equalizes the expression of X-linked genes between males (XY) and females (XX), and in Drosophila is achieved by hypertranscription of the single male X chromosome by the dosage compensation complex (DCC), a ribonucleoprotein assembly of at least five proteins (MSL1, MSL2, MSL3, MOF, and MLE) and two noncoding RNAs (roX1 and roX2) (Gelbart and Kuroda 2009). In females, UNR binds to msl2 mRNA and inhibits its translation, contributing to repressing dosage compensation Duncan et al 2006;Patalano et al 2009). Binding of UNR to msl2 mRNA depends on the female-specific RBP Sex-lethal (SXL), which, in addition to recruiting UNR to the 39 UTR of msl2, promotes the retention of a facultative intron in msl2 59 UTR (for review, see Graindorge et al 2011).…”

Section: Introductionmentioning

confidence: 99%

“…In males, UNR does not bind to msl2 because SXL is absent. In contrast, UNR binds to the roX RNAs in males, and this binding may contribute to promoting DCC recruitment to the X chromosome (Patalano et al 2009). …”

Section: Introductionmentioning

confidence: 99%

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Widespread generation of alternative UTRs contributes to sex-specific RNA binding by UNR

Mihailovich

Wurth

Zambelli

et al. 2011

RNA

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Upstream of N-ras (UNR) is a conserved RNA-binding protein that regulates mRNA translation and stability by binding to sites generally located in untranslated regions (UTRs). In Drosophila, sex-specific binding of UNR to msl2 mRNA and the noncoding RNA roX is believed to play key roles in the control of X-chromosome dosage compensation in both sexes. To investigate broader sex-specific functions of UNR, we have identified its RNA targets in adult male and female flies by high-throughput RNA binding and transcriptome analysis. Here we show that UNR binds to a large set of protein-coding transcripts and to a smaller set of noncoding RNAs in a sex-specific fashion. The analyses also reveal a strong correlation between sex-specific binding of UNR and sex-specific differential expression of UTRs in target genes. Validation experiments indicate that UNR indeed recognizes sex-specifically processed transcripts. These results suggest that UNR exploits the transcript diversity generated by alternative processing and alternative promoter usage to bind and regulate target genes in a sex-specific manner.

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Section: Identification Of Unr Targetsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Widespread generation of alternative UTRs contributes to sex-specific RNA binding by UNR

Mihailovich

Wurth

Zambelli

et al. 2011

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“…9). In males, UNR promotes the targeting of the MSL-DCC to the X-chromosome by a poorly understood mechanism that does not involve translational regulation of MSL proteins 10 . UNR-dependent regulation can be recapitulated in male S2 cells, which express only roX2 (ref.…”

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UNR facilitates the interaction of MLE with the lncRNA roX2 during Drosophila dosage compensation

et al. 2014

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Dosage compensation is a regulatory process that balances the expression of X-chromosomal genes between males (XY) and females (XX). In Drosophila, this requires non-coding RNAs and RNA-binding proteins (RBPs) whose specific functions remain elusive. Here we show that the Drosophila RBP UNR promotes the targeting of the activating male-specific-lethal complex to the X-chromosome by facilitating the interaction of two crucial subunits: the RNA helicase MLE and the long non-coding RNA roX2.

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“…However, Unr also has a function in male flies to promote dosage compensation; the mechanism of this positive role is not clear, but may involve interactions with the non-coding roX RNAs that both bind Unr and are part of the DCC. 5 Anna Bremer (Leibniz Institute for Age Research-Fritz Lipmann Institute, Germany) presented data on the RING finger protein TRIM37, whose mutation causes the disorder Mulibrey nanism. 6 Binding of TRIM37 to the 3'UTR of the CCAAT/enhancer-binding protein (C/EBP) α stimulated the translation of a truncated C/EBPα isoform that promotes proliferation.…”

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Dual sex-specific functions ofDrosophilaUpstream of N-ras in the control of X chromosome dosage compensation

Cited by 24 publications

References 44 publications

Widespread generation of alternative UTRs contributes to sex-specific RNA binding by UNR

Widespread generation of alternative UTRs contributes to sex-specific RNA binding by UNR

UNR facilitates the interaction of MLE with the lncRNA roX2 during Drosophila dosage compensation

Tapas and RNA in Renaissance Spain

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