Age‐dependent integrity of the meiotic spindle assembly checkpoint in females requires Aurora kinase B

Blengini, Cecilia S.; Nguyen, Alexandra L.; Aboelenain, Mansour; Schindler, Karen

doi:10.1111/acel.13489

Cited by 20 publications

(17 citation statements)

References 55 publications

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“…The SAC is desensitized during oocyte meiosis, permitting chromosomal segregation in the presence of several chromosomal misarrangements [27]. Even though the SAC was induced during meiosis, almost 44% of HtrA2-KD oocytes extruded the rst polar body (Fig.…”

Section: Htra2 Knockdown Causes Cytoskeletal Disorganization In Young...mentioning

confidence: 97%

“…Given that decreased HtrA2 expression impeded extrusion of the rst polar body, we hypothesized that HtrA2 might be involved in spindle organization or migration during meiosis. During this process, the SAC acts as a safety mechanism, which holds the oocyte in the metaphase-to-anaphase transition of meiotic phase I until all chromosomes are aligned and microtubules have been correctly attached [27]. Given the arrest in MI of HtrA2-KD young oocytes, we hypothesized potential activation of the SAC.…”

Section: Htra2 Knockdown Activates the Sac In Young Mouse Oocytesmentioning

confidence: 99%

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Insufficient HtrA2 causes meiotic defects by inducing cytoskeletal disorganization in aging germinal vesicle oocytes

Gao

Qiu

Cao

et al. 2022

Preprint

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Background High-temperature requirement protease A2 (HtrA2/Omi) is a mitochondrial chaperone highly conserved from bacteria to humans. It plays an important role in mitochondrial homeostasis and apoptosis. In this study, we investigated the role of HtrA2 in mouse oocyte maturation. Methods The role of HtrA2 in mouse oocyte maturation was investigated by employing knockdown (KD) or overexpression (OE) of HtrA2 in young or old GV oocytes. We employed immunoblotting, immunostaining, fluorescent intensity quantification to test the HtrA2 knockdown on the GV oocyte maturation progression, spindle assembly checkpoint, mitochondrial distribution, spindle assembly, chromosome alignment, actin polymerization, DNA damage and chromosome numbers, the level of acetylated tubulin. Results We observed a significant reduction in HtrA2 protein levels in aging germinal vesicle (GV) oocytes. Young oocytes with low levels of HtrA2 due to siRNA knockdown were unable to complete meiosis and were partially blocked at metaphase I (MI). They also displayed significantly more BubR1 on kinetochores, indicating that the spindle assembly checkpoint was triggered at MI. Extrusion of the first polar body (Pb1) was significantly less frequent and oocytes with large polar bodies were observed when HtrA2 was depleted. In addition, HtrA2 knockdown induced meiotic spindle/chromosome disorganization, leading to aneuploidy at metaphase II (MII), possibly due to the elevated level of acetylated tubulin. Importantly, overexpression of HtrA2 partially rescued spindle/chromosome disorganization and reduced the rate of aneuploidy in aging oocytes. Conclusions Collectively, our data suggest that HtrA2 is a key regulator of oocyte maturation, and its deficiency with age appears to contribute to reproduction failure in females.

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Section: Htra2 Knockdown Causes Cytoskeletal Disorganization In Young...mentioning

confidence: 97%

Section: Htra2 Knockdown Activates the Sac In Young Mouse Oocytesmentioning

confidence: 99%

Insufficient HtrA2 causes meiotic defects by inducing cytoskeletal disorganization in aging germinal vesicle oocytes

Gao

Qiu

Cao

et al. 2022

Preprint

View full text Add to dashboard Cite

show abstract

“…The SAC is triggered by unattached kinetochores. In a recent study on mice oocytes, it was revealed that AURKB appears to play a role in the maintenance of the female reproductive lifespan, most likely because of its defensive property against the excessive accumulation of reactive oxygen species in the egg [ 51 ]. However, this is only one possible factor among others.…”

Section: Effect Of Advanced Maternal Age On Chromosomal Segregation A...mentioning

confidence: 99%

“…However, this is only one possible factor among others. Therefore, further investigations on the abundance of AURKB with respect to the advancing age of the egg could shed light on its ability to be used as an adequate biomarker for oocyte developmental competence in women with aging-related decreases in fertility [ 51 ].…”

Section: Effect Of Advanced Maternal Age On Chromosomal Segregation A...mentioning

confidence: 99%

Chromosome Segregation in the Oocyte: What Goes Wrong during Aging

Wasielak-Politowska¹,

Kordowitzki

2022

IJMS

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Human female fertility and reproductive lifespan decrease significantly with age, resulting in an extended post-reproductive period. The central dogma in human female reproduction contains two important aspects. One is the pool of oocytes in the human ovary (the ovarian reserve; approximately 106 at birth), which diminishes throughout life until menopause around the age of 50 (approximately 103 oocytes) in women. The second is the quality of oocytes, including the correctness of meiotic divisions, among other factors. Notably, the increased rate of sub- and infertility, aneuploidy, miscarriages, and birth defects are associated with advanced maternal age, especially in women above 35 years of age. This postponement is also relevant for human evolution; decades ago, the female aging-related fertility drop was not as important as it is today because women were having their children at a younger age. Spindle assembly is crucial for chromosome segregation during each cell division and oocyte maturation, making it an important event for euploidy. Consequently, aberrations in this segregation process, especially during the first meiotic division in human eggs, can lead to implantation failure or spontaneous abortion. Today, human reproductive medicine is also facing a high prevalence of aneuploidy, even in young females. However, the shift in the reproductive phase of humans and the strong increase in errors make the problem much more dramatic at later stages of the female reproductive phase. Aneuploidy in human eggs could be the result of the non-disjunction of entire chromosomes or sister chromatids during oocyte meiosis, but partial or segmental aneuploidies are also relevant. In this review, we intend to describe the relevance of the spindle apparatus during oocyte maturation for proper chromosome segregation in the context of maternal aging and the female reproductive lifespan.

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“…AURKC is responsible for most functions that AURKB-CPC has in mitosis [ 8 , 9 ], including regulating chromosome alignment and correcting erroneous kinetochore-microtubule attachments [ 10 – 12 ]. As a result, AURKB is diffuse in the oocyte cytoplasm and has still to be defined mechanisms in protecting egg quality with age [ 13 , 14 ]. Therefore, subcellular localization and function of AURKA and AURKC in mouse oocytes is dictated by their binding to different activators as in mitotic cells.…”

Section: Introductionmentioning

confidence: 99%

Using ZINC08918027 inhibitor to determine Aurora kinase-chromosomal passenger complex isoforms in mouse oocytes

et al. 2022

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Objective Miscarriages affect 10% of women aged 25–29, and 53% of women over 45. The primary cause of miscarriage is aneuploidy that originated in eggs. The Aurora kinase family has three members that regulate chromosome segregation. Therefore, distinguishing the roles of these isoforms is important to understand aneuploidy etiology. In meiosis, Aurora kinase A (AURKA) localizes to spindle poles, where it binds TPX2. Aurora kinase C (AURKC) localizes on chromosomes, where it replaces AURKB as the primary AURK in the chromosomal passenger complex (CPC) via INCENP binding. Although AURKA compensates for CPC function in oocytes lacking AURKB/C, it is unknown whether AURKA binds INCENP in wild type mouse oocytes. ZINC08918027 (ZC) is an inhibitor that prevents the interaction between AURKB and INCENP in mitotic cells. We hypothesized that ZC would block CPC function of any AURK isoform. Results ZC treatment caused defects in meiotic progression and spindle building. By Western blotting and immunofluorescence, we observed that activated AURKA and AURKC levels in ZC-treated oocytes decreased compared to controls. These results suggest there is a population of AURKA-CPC in mouse oocytes. These data together suggest that INCENP-dependent AURKA and AURKC activities are needed for spindle bipolarity and meiotic progression.

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Age‐dependent integrity of the meiotic spindle assembly checkpoint in females requires Aurora kinase B

Cited by 20 publications

References 55 publications

Insufficient HtrA2 causes meiotic defects by inducing cytoskeletal disorganization in aging germinal vesicle oocytes

Insufficient HtrA2 causes meiotic defects by inducing cytoskeletal disorganization in aging germinal vesicle oocytes

Chromosome Segregation in the Oocyte: What Goes Wrong during Aging

Using ZINC08918027 inhibitor to determine Aurora kinase-chromosomal passenger complex isoforms in mouse oocytes

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