Meiotic non-disjunction mechanisms in human fertile males

Uroz, Laia; Templado, C.

doi:10.1093/humrep/des051

Cited by 21 publications

(16 citation statements)

References 43 publications

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“…48). Trisomy 21 pregnancies (95%) are due to errors in female meiosis 48 , whereas errors in chromosome segregation in male meiosis are much lower, being around 2.5% for autosomes 49 . Unlike meiotic divisions in males, which take place immediately after pachytene and successful recombination, female meiosis comes to a halt for weeks or months (in mice) or decades (in humans) in prophase I, before meiosis is resumed to give rise to one or more fertilizable eggs.…”

Section: Discussionmentioning

confidence: 99%

Mouse oocytes depend on BubR1 for proper chromosome segregation but not for prophase I arrest

et al. 2015

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Mammalian female meiosis is error prone, with rates of meiotic chromosome missegregations strongly increasing towards the end of the reproductive lifespan. A strong reduction of BubR1 has been observed in oocytes of women approaching menopause and in ovaries of aged mice, which led to the hypothesis that a gradual decline of BubR1 contributes to age-related aneuploidization. Here we employ a conditional knockout approach in mouse oocytes to dissect the meiotic roles of BubR1. We show that BubR1 is required for diverse meiotic functions, including persistent spindle assembly checkpoint activity, timing of meiosis I and the establishment of robust kinetochore-microtubule attachments in a meiosis-specific manner, but not prophase I arrest. These data reveal that BubR1 plays a multifaceted role in chromosome segregation during the first meiotic division and suggest that age-related decline of BubR1 is a key determinant of the formation of aneuploid oocytes as women approach menopause.

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Section: Discussionmentioning

confidence: 99%

Mouse oocytes depend on BubR1 for proper chromosome segregation but not for prophase I arrest

et al. 2015

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“…Our results indicated such a frequency at 2.31%, while three other cases of three-way CCR analyses found it to be 9.3% (Loup et al 2010), 3.15% (Pellestor et al 2011b) and 15.6% (Godo et al 2013). Unexpected FISH phenotypes can be the consequence of three factors: i) nondisjunction at the second meiotic division, ii) increasing difficulty in FISH result interpretation with increasing number of chromosomes involved, and iii) possible chiasma occurrence, leading to the formation of additional recombinant chromosomes (Anton et al 2007, Uroz & Templado 2012. In cases of three-way der (6) der (10) 10 6 11 der (11) q25.1 q24.3 q23.1 Figure 3 Schematic model of the suggested hexavalent configuration during the pachytene stage in meiosis I in a 46,XY,t(6;10;11)(q25.1;q24.3;q23.1)mat carrier.…”

Section: Discussionmentioning

confidence: 92%

Sperm FISH and chromatin integrity in spermatozoa from a t(6;10;11) carrier

Olszewska

Huleyuk²,

Frączek³

et al. 2014

Reproduction

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Complex chromosome rearrangements (CCRs) are structurally balanced or unbalanced aberrations involving more than two breakpoints on two or more chromosomes. CCRs can be a potential reason for genomic imbalance in gametes, which leads to a drastic reduction in fertility. In this study, the meiotic segregation pattern, aneuploidy of seven chromosomes uninvolved in the CCR and chromatin integrity were analysed in the ejaculated spermatozoa of a 46,XY,t(6;10;11)(q25.1;q24.3;q23.1)mat carrier with asthenozoospermia and a lack of conception. The frequency of genetically unbalanced spermatozoa was 78.8% with a prevalence of 4:2 segregants of 38.2%, while the prevalence of the adjacent 3:3 mode was 35.3%. Analysis of the aneuploidy of chromosomes 13, 15, 18, 21, 22, X and Y revealed an approximately fivefold increased level in comparison with that of the control group, indicating the presence of an interchromosomal effect. Sperm chromatin integrity status was evaluated using chromomycin A3 and aniline blue staining (deprotamination), acridine orange test and TUNEL assay (sperm DNA fragmentation). No differences were found when comparisons were made with a control group. We suggest that the accumulation of genetically unbalanced spermatozoa, significantly increased sperm aneuploidy level and decreased sperm motility (20%, progressive) were not responsible for the observed lack of reproductive success in the analysed infertile t(6;10;11) carrier. Interestingly, in the case described herein, a high level of sperm chromosomal imbalance appears not to be linked to sperm chromatin integrity status.

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“…Studies conducted to date have shown that the overall disomy frequencies observed in spermatocytes II are significantly higher than those observed in mature human spermatozoa, suggesting the existence of effective, post‐meiotic checkpoint mechanisms that monitor and arrest spermatocytes II with numerical abnormalities. Inefficient control mechanisms could, therefore, be one explanation for the increased rate of chromosome abnormalities observed in the spermatozoa of certain male subgroups (Uroz & Templado, ).…”

Section: Resultsmentioning

confidence: 99%

Sperm aneuploidy in infertile male patients: a systematic review of the literature

Chatziparasidou

Christoforidis

Samolada³

et al. 2014

Andrologia

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Males with abnormal karyotypes and subgroups of fertile and infertile males with normal karyotypes may be at risk of producing unbalanced or aneuploid spermatozoa. Biological, clinical, environmental and other factors may also cause additional sperm aneuploidy. However, increased risk of sperm aneuploidy is directly related to chromosomally abnormal embryo production and hence to poor reproductive potential. This systemic literature review focuses on the identification of these males because this is an essential step in the context of assisted reproduction. This research may allow for a more personalised and, hence, more accurate estimation of the risk involved in each case, which in turn will aid genetic counselling for affected couples and help with informed decision-making.

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Meiotic non-disjunction mechanisms in human fertile males

Cited by 21 publications

References 43 publications

Mouse oocytes depend on BubR1 for proper chromosome segregation but not for prophase I arrest

Mouse oocytes depend on BubR1 for proper chromosome segregation but not for prophase I arrest

Sperm FISH and chromatin integrity in spermatozoa from a t(6;10;11) carrier

Sperm aneuploidy in infertile male patients: a systematic review of the literature

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