Ectopic assembly of heterochromatin in
            <i>Drosophila melanogaster</i>
            triggered by transposable elements

Sentmanat, Monica F.; Elgin, Sarah C. R.

doi:10.1073/pnas.1207036109

Cited by 82 publications

(112 citation statements)

References 43 publications

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“…Similarly, in Drosophila, two distinct RNAi-like processes for silencing Tns have been elucidated. In the germline, the Piwi-interacting RNA (piRNA) pathway generates small RNAs that suppress Tns by inducing heterochromatin formation (Vagin et al 2006;Aravin et al 2007;Brennecke et al 2007;Sentmanat and Elgin 2012;Le Thomas et al 2013). In somatic cells, esiRNAs silence retroTns via a Dicer 2 (Dcr-2)/Argonaute 2 (Ago2)-dependent mechanism (Chung et al 2008;Czech et al 2008;Ghildiyal et al 2008;Saito and Siomi 2010;Xie et al 2013).…”

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confidence: 99%

Antisense Transcription of Retrotransposons in Drosophila: An Origin of Endogenous Small Interfering RNA Precursors

2015

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Movement of transposons causes insertions, deletions, and chromosomal rearrangements potentially leading to premature lethality in Drosophila melanogaster. To repress these elements and combat genomic instability, eukaryotes have evolved several small RNA-mediated defense mechanisms. Specifically, in Drosophila somatic cells, endogenous small interfering (esi)RNAs suppress retrotransposon mobility. EsiRNAs are produced by Dicer-2 processing of double-stranded RNA precursors, yet the origins of these precursors are unknown. We show that most transposon families are transcribed in both the sense (S) and antisense (AS) direction in Dmel-2 cells. LTR retrotransposons Dm297, mdg1, and blood, and non-LTR retrotransposons juan and jockey transcripts, are generated from intraelement transcription start sites with canonical RNA polymerase II promoters. We also determined that retrotransposon antisense transcripts are less polyadenylated than sense. RNA-seq and small RNA-seq revealed that Dicer-2 RNA interference (RNAi) depletion causes a decrease in the number of esiRNAs mapping to retrotransposons and an increase in expression of both S and AS retrotransposon transcripts. These data support a model in which double-stranded RNA precursors are derived from convergent transcription and processed by Dicer-2 into esiRNAs that silence both sense and antisense retrotransposon transcripts. Reduction of sense retrotransposon transcripts potentially lowers element-specific protein levels to prevent transposition. This mechanism preserves genomic integrity and is especially important for Drosophila fitness because mobile genetic elements are highly active.

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Antisense Transcription of Retrotransposons in Drosophila: An Origin of Endogenous Small Interfering RNA Precursors

2015

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“…Most piRNA sequences in the Drosophila genome map to heterochromatic regions (Saito et al 2006), and several lines of investigation have demonstrated that Piwi and HP1a can physically interact (Brower-Toland et al 2007;Mendez et al 2011). Moreover, transcriptional silencing of retrotransposons by the Piwi-piRNA system involves recruitment of HP1a to transposable elements (Wang and Elgin 2011;Sentmanat and Elgin 2012;Huang et al 2013). Piwi also participates in activities that are not directly related to transposon silencing.…”

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confidence: 99%

Heterochromatin-Associated Proteins HP1a and Piwi Collaborate to Maintain the Association of Achiasmate Homologs in Drosophila Oocytes

Giauque¹,

Bickel

2016

Genetics

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Accurate segregation of homologous chromosomes during meiosis depends on their ability to remain physically connected throughout prophase I. For homologs that achieve a crossover, sister chromatid cohesion distal to the chiasma keeps them attached until anaphase I. However, in Drosophila melanogaster wild-type oocytes, chromosome 4 never recombines, and the X chromosome fails to cross over in 6-10% of oocytes. Proper segregation of these achiasmate homologs relies on their pericentric heterochromatin-mediated association, but the mechanism(s) underlying this attachment remains poorly understood. Using an inducible RNA interference (RNAi) strategy combined with fluorescence in situ hybridization (FISH) to monitor centromere proximal association of the achiasmate FM7a/X homolog pair, we asked whether specific heterochromatin-associated proteins are required for the association and proper segregation of achiasmate homologs in Drosophila oocytes. When we knock down HP1a, H3K9 methytransferases, or the HP1a binding partner Piwi during mid-prophase, we observe significant disruption of pericentric heterochromatin-mediated association of FM7a/X homologs. Furthermore, for both HP1a and Piwi knockdown oocytes, transgenic coexpression of the corresponding wild-type protein is able to rescue RNAi-induced defects, but expression of a mutant protein with a single amino acid change that disrupts the HP1a-Piwi interaction is unable to do so. We show that Piwi is stably bound to numerous sites along the meiotic chromosomes, including centromere proximal regions. In addition, reduction of HP1a or Piwi during meiotic prophase induces a significant increase in FM7a/X segregation errors. We present a speculative model outlining how HP1a and Piwi could collaborate to keep achiasmate chromosomes associated in a homology-dependent manner.

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“…A careful examination of this domain revealed a correlation between the presence of the repetitive element 1360 and the variegating phenotype (Sun et al 2004). Follow-up studies found that incorporating 1360 sequences into the hsp70-white transgene construct could increase the gene silencing observed at a subset of insertion sites (Haynes et al 2006;Sentmanat and Elgin 2012). However, these studies also showed that the presence of 1360 was not sufficient to induce PEV-and heterochromatin formation-in general, as full expression, rather than variegation, is observed for insertions of the 1360-hsp70-white transgene at most sites in the euchromatic chromosome arms (Haynes et al 2006;Sentmanat and Elgin 2012).…”

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“…Follow-up studies found that incorporating 1360 sequences into the hsp70-white transgene construct could increase the gene silencing observed at a subset of insertion sites (Haynes et al 2006;Sentmanat and Elgin 2012). However, these studies also showed that the presence of 1360 was not sufficient to induce PEV-and heterochromatin formation-in general, as full expression, rather than variegation, is observed for insertions of the 1360-hsp70-white transgene at most sites in the euchromatic chromosome arms (Haynes et al 2006;Sentmanat and Elgin 2012).The available data suggest that PEV is caused by spreading of adjacent heterochromatin to encompass the reporter gene (Weiler and Wakimoto 1995;Vogel et al 2009). The effectiveness of this spreading is thought to be stochastic, thus leading to the variegating phenotype.…”

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confidence: 99%

“…The effectiveness of this spreading is thought to be stochastic, thus leading to the variegating phenotype. As noted above, proximity to high repeat density regions is key, even if a repeated element such as 1360 is included in the transgene (Wallrath and Elgin 1995;Sun et al 2000;Haynes et al 2006;Sentmanat and Elgin 2012). While the importance of a high density of repetitive elements is well supported, genetic evidence indicates that there are several different mechanisms operating in the various heterochromatic domains of the Drosophila genome (Phalke et al 2009).…”

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confidence: 99%

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Targeting of P-Element Reporters to Heterochromatic Domains by Transposable Element 1360 in Drosophila melanogaster

et al. 2015

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Heterochromatin is a common DNA packaging form employed by eukaryotes to constitutively silence transposable elements. Determining which sequences to package as heterochromatin is vital for an organism. Here, we use Drosophila melanogaster to study heterochromatin formation, exploiting position-effect variegation, a process whereby a transgene is silenced stochastically if inserted in proximity to heterochromatin, leading to a variegating phenotype. Previous studies identified the transposable element 1360 as a target for heterochromatin formation. We use transgene reporters with either one or four copies of 1360 to determine if increasing local repeat density can alter the fraction of the genome supporting heterochromatin formation. We find that including 1360 in the reporter increases the frequency with which variegating phenotypes are observed. This increase is due to a greater recovery of insertions at the telomereassociated sequences (50% of variegating inserts). In contrast to variegating insertions elsewhere, the phenotype of telomere-associated sequence insertions is largely independent of the presence of 1360 in the reporter. We find that variegating and fully expressed transgenes are located in different types of chromatin and that variegating reporters in the telomere-associated sequences differ from those in pericentric heterochromatin. Indeed, chromatin marks at the transgene insertion site can be used to predict the eye phenotype. Our analysis reveals that increasing the local repeat density (via the transgene reporter) does not enlarge the fraction of the genome supporting heterochromatin formation. Rather, additional copies of 1360 appear to target the reporter to the telomere-associated sequences with greater efficiency, thus leading to an increased recovery of variegating insertions. KEYWORDS heterochromatin; transposable elements; position-effect variegation; chromatin; Drosophila I N vivo regulation of gene expression occurs in the context of chromatin, the complex structure formed by DNA, histones, and a variety of associated proteins. Two basic types of chromatin were originally distinguished, euchromatin and heterochromatin, based on cytological staining behavior during the cell cycle (Heitz 1928). Euchromatin and heterochromatin differ in a number of characteristics, including biochemical makeup and their effect on the expression of transgene reporters. Euchromatin is generally accessible for transcription, contains the majority of the genes, and is characterized by biochemical marks associated with transcription, such as high levels of histone acetylation, transcriptional activators, and RNA polymerase II. In contrast, heterochromatin contains few genes and has a high repeat density. Heterochromatin is characterized by low levels of histone acetylation, high levels of histone 3 lysine 9 (H3K9) methylation, and the presence of "silencing" proteins such as heterochromatin protein 1 (HP1) (Beisel and Paro 2011). While this model of two basic chromatin types has been very successful...

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Ectopic assembly of heterochromatin in Drosophila melanogaster triggered by transposable elements

Cited by 82 publications

References 43 publications

Antisense Transcription of Retrotransposons in Drosophila: An Origin of Endogenous Small Interfering RNA Precursors

Antisense Transcription of Retrotransposons in Drosophila: An Origin of Endogenous Small Interfering RNA Precursors

Heterochromatin-Associated Proteins HP1a and Piwi Collaborate to Maintain the Association of Achiasmate Homologs in Drosophila Oocytes

Targeting of P-Element Reporters to Heterochromatic Domains by Transposable Element 1360 in Drosophila melanogaster

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