p53 is required for female germline stem cell maintenance in P-element hybrid dysgenesis

Tasnim, Sadia; Kelleher, Erin S.

doi:10.1016/j.ydbio.2017.12.021

Cited by 24 publications

(35 citation statements)

References 40 publications

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“…Ectopic recombination events between TE insertions in different genomic locations further produce large structural rearrangements, duplications, and deletions, which are overwhelmingly deleterious (reviewed in Hedges and Deininger, 2007). In addition to these mutational impacts, TE activity itself can have drastic fitness consequences by causing dysgenic sterility, a condition in which germline DNA damage prohibits the production of viable gametes (Bingham et al, 1982;Josefsson et al, 2006;Orsi et al, 2010;Tasnim and Kelleher, 2018). Despite these fitness costs, nearly all genomes are populated by TEs (reviewed in Huang et al, 2012), and…”

Section: Introductionmentioning

confidence: 99%

The Evolution of Small-RNA-Mediated Silencing of an Invading Transposable Element

Kelleher

Azevedo

Zheng

2017

Preprint

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Transposable elements (TEs) are genomic parasites that impose fitness costs on their hosts by producing deleterious mutations and disrupting gametogenesis. Host genomes avoid these costs by regulating TE activity, particularly in germline cells where new insertions are heritable and TEs are exceptionally active. However, the capacity of different TE-associated fitness costs to select for repression in the host, and the role of selection in the evolution of TE regulation more generally, remain controversial. In this study, we use individual-based simulations to examine the evolution of TE regulation through small RNA-mediated silencing. Small RNA silencing is a common mechanism for TE regulation employed by both prokaryotes and eukaryotes. We observed that even under conservative assumptions, where small RNA-mediated regulation reduces transposition only, repression evolves rapidly and adaptively after the genome is invaded by a new TE. We further show that the spread of repressor alleles is greatly enhanced by two additional TE-imposed fitness costs: dysgenic sterility and ectopic recombination. Finally, we demonstrate that the mutation rate to repression (i.e., the size of the mutational target) is a critical parameter that influences both the evolutionary trajectory of host repression and the associated proliferation of TEs. Our findings suggest that adaptive evolution of TE regulation may be stronger and more prevalent than previously suggested, and complement recent empirical observations of positive selection on small RNA-mediated repressor alleles. Both prokaryotic and eukaryotic genomes minimize the fitness costs of TEs by controlling their activity through small RNA mediated silencing (reviewed in Blumenstiel 2011). In eukaryotic germlines, small RNA mediated silencing of TEs is enacted by Argonaute proteins that are found in complex with small interfering RNAs (siRNAs) and Piwi-interacting RNAs (piRNAs). Regulatory siRNAs and piRNAs are produced from anti-sense TE transcripts, and identify TE-derived mRNAs by base complementarity. Complexed Argonaute proteins then silence the targeted TE transcriptionally by inducing heterochromatin formation, or post-transcriptionally by degrading the transcript. Consistent with prevention of germline DNA damage, small RNA-mediated silencing suppresses TE-associated dysgenic sterility in Drosophila (Blumenstiel and Hartl 2005;Brennecke et al. 2008;Chambeyron et al. 2008;Rozhkov et al.

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Section: Introductionmentioning

confidence: 99%

The Evolution of Small-RNA-Mediated Silencing of an Invading Transposable Element

Kelleher

Azevedo

Zheng

2017

Preprint

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“…The incomplete penetrance suggests that a pathway active in the HD germline, other than MDRG, is partly responsible for the germline-loss phenotype. Compatible with this, mutation in loki/Chk2 partially suppresses the germline-loss phenotype caused by HD 22 . Therefore, it is reasonable to speculate that at least two germline-elimination mechanisms, MDRG and a Chk2-dependent pathway, are responsible for the HD-induced germline-loss phenotype in females.…”

Section: Discussionmentioning

confidence: 77%

“…Later, in meiotic cells, p53 acts as a downstream effector of loki/Chk2 to induce apoptosis 18,21 . Consistent with their roles in the DNA damage response, loki/Chk2 and p53 also act as modifiers of HDcaused germline loss during oogenesis 22 . Although there is no known link between DNA damage response and Bruno, a regulator of oogenesis [23][24][25] , Bruno activity is also required for the GSC loss phenotype in adult HD females 26 .…”

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confidence: 70%

“…Because it is thought that DNA damage associated with HD causes the germline-loss phenotype 17,40 , one possible mechanism underlying MDRG is that Myc mediates DDR, which induces cell-cycle arrest and apoptosis in the germline 41,42 . In Drosophila oogenesis, when female GSCs and their daughter cells are exposed to DNA damage, loki/Chk2 is required for cell-cycle arrest of GSCs and the loss of these cells 20,22 . Moreover, in meiotic cells, p53 acts downstream of loki/Chk2 to induce apoptosis in response to DNA damage 18,21 .…”

Section: Discussionmentioning

confidence: 99%

“…Moreover, in meiotic cells, p53 acts downstream of loki/Chk2 to induce apoptosis in response to DNA damage 18,21 . Thus, germline loss during oogenesis in HD females results from GSC loss and meiotic cell apoptosis, which are caused by DNA damage associated with P-element mobilization 22,26 . However, MDRG occurs in HD females at the early third-instar stage ( Figs.…”

Section: Discussionmentioning

confidence: 99%

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Myc plays an important role in Drosophila P-M hybrid dysgenesis to eliminate germline cells with genetic damage

Ota

Kobayashi

2020

Commun Biol

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Genetic damage in the germline induced by P-element mobilization causes a syndrome known as P-M hybrid dysgenesis (HD), which manifests as elevated mutation frequency and loss of germline cells. In this study, we found that Myc plays an important role in eliminating germline cells in the context of HD. P-element mobilization resulted in downregulation of Myc expression in the germline. Myc knockdown caused germline elimination; conversely, Myc overexpression rescued the germline loss caused by P-element mobilization. Moreover, restoration of fertility by Myc resulted in the production of gametes with elevated mutation frequency and reduced ability to undergo development. Our results demonstrate that Myc downregulation mediates elimination of germline cells with accumulated genetic damage, and that failure to remove these cells results in increased production of aberrant gametes. Therefore, we propose that elimination of germline cells mediated by Myc downregulation is a quality control mechanism that maintains the genomic integrity of the germline.

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Transposable elements and their role in aging

Yushkova

Moskalev

2023

Ageing Research Reviews

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p53 is required for female germline stem cell maintenance in P-element hybrid dysgenesis

Cited by 24 publications

References 40 publications

The Evolution of Small-RNA-Mediated Silencing of an Invading Transposable Element

The Evolution of Small-RNA-Mediated Silencing of an Invading Transposable Element

Myc plays an important role in Drosophila P-M hybrid dysgenesis to eliminate germline cells with genetic damage

Transposable elements and their role in aging

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