Inactivation or non-reactivation: what accounts better for the silence of sex chromosomes during mammalian male meiosis?

Page, Jesús; Fuente, Roberto de la; Manterola, Marcia; Parra, María Teresa; Viera, Alberto; Berríos, Soledad; Fernández-Donoso, Raúl; Rufas, Julio S.

doi:10.1007/s00412-012-0364-y

Cited by 94 publications

(167 citation statements)

References 82 publications

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“…RNAs to the sex body (Page et al, 2012). However, an alternative possibility recently proposed assumes that MSCI represents the maintenance of a prior repressed state (Page et al, 2012).…”

Section: Smc5/6 Complexes At the Sex Bodymentioning

confidence: 99%

Dynamic localization of SMC5/6 complex proteins during mammalian meiosis and mitosis implies functions in distinct chromosome processes

Gómez

Jordan

Viera

et al. 2013

Journal of Cell Science

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SummaryFour members of the structural maintenance of chromosome (SMC) protein family have essential functions in chromosome condensation (SMC2/4) and sister-chromatid cohesion (SMC1/3). The SMC5/6 complex has been implicated in chromosome replication, DNA repair and chromosome segregation in somatic cells, but its possible functions during mammalian meiosis are unknown. Here, we show in mouse spermatocytes that SMC5 and SMC6 are located at the central region of the synaptonemal complex from zygotene until diplotene. During late diplotene both proteins load to the chromocenters, where they colocalize with DNA Topoisomerase IIa, and then accumulate at the inner domain of the centromeres during the first and second meiotic divisions. Interestingly, SMC6 and DNA Topoisomerase IIa colocalize at stretched strands that join kinetochores during the metaphase II to anaphase II transition, and both are observed on stretched lagging chromosomes at anaphase II following treatment with Etoposide. During mitosis, SMC6 and DNA Topoisomerase IIa colocalize at the centromeres and chromatid axes. Our results are consistent with the participation of SMC5 and SMC6 in homologous chromosome synapsis during prophase I, chromosome and centromere structure during meiosis I and mitosis and, with DNA Topoisomerase IIa, in regulating centromere cohesion during meiosis II.

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“…RNAs to the sex body (Page et al, 2012). However, an alternative possibility recently proposed assumes that MSCI represents the maintenance of a prior repressed state (Page et al, 2012).…”

Section: Smc5/6 Complexes At the Sex Bodymentioning

confidence: 99%

Dynamic localization of SMC5/6 complex proteins during mammalian meiosis and mitosis implies functions in distinct chromosome processes

Gómez

Jordan

Viera

et al. 2013

Journal of Cell Science

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“…In mammals, the phosphorylated form of histone H2AX (gH2AX) is one of the characteristic responses to this damage, and thus it is used as a common marker of DNA damage during meiosis (Mahadevaiah et al 2001). Additionally, gH2AX is accumulated on sex chromosomes from pachytene up to metaphase I, where it functions in the meiotic silencing of sex chromosomes (Mahadevaiah et al 2001;Turner et al 2004;Page et al 2012).We followed the location of gH2AX during pachytene in combination with labeling of the centromeres to ascertain if the centromeres were specifically marked for DNA damage and repair during these stages (Figure 6, A-D). We found that during early pachytene gH2AX was abundantly distributed on the sex chromosomes, which showed a fuzzy appearance ( Figure 6A).…”

Section: Dna Damage-response Proteins Do Not Specifically Associate Wmentioning

confidence: 99%

“…It is then possible that the particular dynamics that RAP1 and TRF1 exhibit during prophase I could be related to protection and integrity maintenance of the ITSs, especially from pachytene up to diplotene, when chromatin in autosomes becomes decondensed and transcriptionally active (Page et al 2012). This becomes particularly important since meiosis is a critical process for genome stability.…”

Section: Structural Organization Of Its Chromatin During Meiosismentioning

confidence: 99%

Chromatin Organization and Remodeling of Interstitial Telomeric Sites During Meiosis in the Mongolian Gerbil (Meriones unguiculatus)

et al. 2014

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Telomeric DNA repeats are key features of chromosomes that allow the maintenance of integrity and stability in the telomeres. However, interstitial telomere sites (ITSs) can also be found along the chromosomes, especially near the centromere, where they may appear following chromosomal rearrangements like Robertsonian translocations. There is no defined role for ITSs, but they are linked to DNA damage-prone sites. We were interested in studying the structural organization of ITSs during meiosis, a kind of cell division in which programmed DNA damage events and noticeable chromatin reorganizations occur. Here we describe the presence of highly amplified ITSs in the pericentromeric region of Mongolian gerbil (Meriones unguiculatus) chromosomes. During meiosis, ITSs show a different chromatin conformation than DNA repeats at telomeres, appearing more extended and accumulating heterochromatin markers. Interestingly, ITSs also recruit the telomeric proteins RAP1 and TRF1, but in a stage-dependent manner, appearing mainly at late prophase I stages. We did not find a specific accumulation of DNA repair factors to the ITSs, such as gH2AX or RAD51 at these stages, but we could detect the presence of MLH1, a marker for reciprocal recombination. However, contrary to previous reports, we did not find a specific accumulation of crossovers at ITSs. Intriguingly, some centromeric regions of metacentric chromosomes may bind the nuclear envelope through the association to SUN1 protein, a feature usually performed by telomeres. Therefore, ITSs present a particular and dynamic chromatin configuration in meiosis, which could be involved in maintaining their genetic stability, but they additionally retain some features of distal telomeres, provided by their capability to associate to telomere-binding proteins.

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“…This post-translational modification of histone H2AX is believed to trigger a positive feedback loop between H2AX and MDC1 to promote the additional recruitment of epigenetic factors responsible for silencing the sex chromosomes during meiosis (FernandezCapetillo et al, 2003;Ichijima et al, 2011). It has been reported that molecular events leading to MSCI are initiated at the zygotene to pachytene transition during prophase I in spermatocytes, and that the actual gene silencing effects are first manifest at the early pachytene stage (Page et al, 2012;Royo et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

Escape of X-linked miRNA genes from meiotic sex chromosome inactivation

et al. 2015

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Past studies have indicated that transcription of all X-linked genes is repressed by meiotic sex chromosome inactivation (MSCI) during the meiotic phase of spermatogenesis in mammals. However, more recent studies have shown an increase in steady-state levels of certain X-linked miRNAs in pachytene spermatocytes, suggesting that either synthesis of these miRNAs increases or that degradation of these miRNAs decreases dramatically in these cells. To distinguish between these possibilities, we performed RNA-FISH to detect nascent transcripts from multiple miRNA genes in various spermatogenic cell types. Our results show definitively that Type I X-linked miRNA genes are subject to MSCI, as are all or most X-linked mRNA genes, whereas Type II and III X-linked miRNA genes escape MSCI by continuing ongoing, active transcription in primary spermatocytes. We corroborated these results by co-localization of RNA-FISH signals with both a corresponding DNA-FISH signal and an immunofluorescence signal for RNA polymerase II. We also found that X-linked miRNA genes that escape MSCI locate non-randomly to the periphery of the XY body, whereas genes that are subject to MSCI remain located within the XY body in pachytene spermatocytes, suggesting that the mechanism of escape of X-linked miRNA genes from MSCI involves their relocation to a position outside of the repressive chromatin domain associated with the XY body. The fact that Type II and III X-linked miRNA genes escape MSCI suggests an immediacy of function of the encoded miRNAs specifically required during the meiotic stages of spermatogenesis.

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Inactivation or non-reactivation: what accounts better for the silence of sex chromosomes during mammalian male meiosis?

Cited by 94 publications

References 82 publications

Dynamic localization of SMC5/6 complex proteins during mammalian meiosis and mitosis implies functions in distinct chromosome processes

Dynamic localization of SMC5/6 complex proteins during mammalian meiosis and mitosis implies functions in distinct chromosome processes

Chromatin Organization and Remodeling of Interstitial Telomeric Sites During Meiosis in the Mongolian Gerbil (Meriones unguiculatus)

Escape of X-linked miRNA genes from meiotic sex chromosome inactivation

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