The Role of Mitochondrial DNA Copy Number in Mammalian Fertility1

Wai, Timothy; Ao, Asangla; Zhang, Xiaoyun; Cyr, Daniel G.; Dufort, Daniel; Shoubridge, Eric A.

doi:10.1095/biolreprod.109.080887

Cited by 366 publications

(339 citation statements)

References 77 publications

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“…Aneuploidy incidence rates increase with age in humans and mice, with evidence suggesting age-related degradation of cohesin proteins in the oocyte nucleus is involved (Chiang et al 2010, Lister et al 2010, Kuliev et al 2011, Duncan et al 2012. Oocyte mitochondrial counts also decline in older females, leading to reduced embryo viability (Wai et al 2010, Kushnir et al 2012, Fragouli et al 2015. Additional factors that contribute to the age-related decline in oocyte quality may yet be discovered, but there is no current evidence to suggest that AMH directly affects oocyte quality.…”

Section: The Effect Of Ovarian Reserve On Declining Fertilitymentioning

confidence: 99%

A putative role for anti-Müllerian hormone (AMH) in optimising ovarian reserve expenditure

Pankhurst

2017

Journal of Endocrinology

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The mammalian ovary has a finite supply of oocytes, which are contained within primordial follicles where they are arrested in a dormant state. The number of primordial follicles in the ovary at puberty is highly variable between females of the same species. Females that enter puberty with a small ovarian reserve are at risk of a shorter reproductive lifespan, as their ovarian reserve is expected to be depleted faster. One of the roles of anti-Müllerian hormone (AMH) is to inhibit primordial follicle activation, which slows the rate at which the ovarian reserve is depleted. A simple interpretation is that the function of AMH is to conserve ovarian reserve. However, the females with the lowest ovarian reserve and the greatest risk of early reserve depletion have the lowest levels of AMH. In contrast, AMH apparently strongly inhibits primordial follicle activation in females with ample ovarian reserve, for reasons that remain unexplained. The rate of primordial follicle activation determines the size of the developing follicle pool, which in turn, determines how many oocytes are available to be selected for ovulation. This review discusses the evidence that AMH regulates the size of the developing follicle pool by altering the rate of primordial follicle activation in a context-dependent manner. The expression patterns of AMH across life are also consistent with changing requirements for primordial follicle activation in the ageing ovary. A potential role of AMH in the fertility of ageing females is proposed herein.

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Section: The Effect Of Ovarian Reserve On Declining Fertilitymentioning

confidence: 99%

A putative role for anti-Müllerian hormone (AMH) in optimising ovarian reserve expenditure

Pankhurst

2017

Journal of Endocrinology

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“…In this sense, the results of Chiaratti et al [13] are consistent with our observations: 1-cell embryos that were able to recover the high mtDNA content removed by centrifugation and advanced to the blastocyst stage, must maintain functional mechanisms of fusion and fission required for the distribution of genetic material. This may also explain on the mouse oocyte model, in which with only 4,000 copies of mtDNA, embryos were able to progress until the blastocyst stage [62].…”

Section: Mitochondriamentioning

confidence: 94%

Does serum cause lipid-droplet accumulation in bovine embryos produced in vitro, during developmental days 1 to 4?

Crocco

Kelmansky

Mariano

2013

J Assist Reprod Genet

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SummaryPurpose Serum supplementation has shown to have beneficial effects on in vitro bovine embryo development. However, it is often assumed that serum supplementation may produce mitochondrial damage and this damage would generate lipid accumulation, a major obstacle for cryopreservation. The aim of the present study is to investigate the previous assumptions in early embryonic stages. Methods We considered in vitro produced bovine embryos from day 1 to 4 of development, which were grown in presence of serum from days 1, 2 or 3 or in absence of it. Electron transmission micrographs allowed us to quantify the area occupied by lipid droplets and by the different mitochondrial types to evaluate serum effect. Using confocal microscopy we analyzed mitochondrial activity and location. Results We found no evidence of lipid droplets accumulation or mitochondrial degeneration or reduction of mitochondrial area in serum supplemented media. Further, our results suggest that events of mitochondrial proliferation are taking place even in serum supplemented media.Conclusions Serum does not produce lipid accumulation or mitochondrial damage in bovine embryos from 2 to 16 cells. When serum was added to embryo culture medium on day 3 of development, there were ultrastructural signs of a beneficial effect for embryo development. The lack of serum until day 3 may also avoid the unnecessary exposure to potentially inhibitory factors present on it.

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“…The presence of mitochondrial dysfunction secondary to mtDNA deletions is tissue‐specific and has been linked to many pathologies, such as diabetes, heart failure, neurodegenerative diseases, and even cancer 42. However, as mtDNA mutations affect only a subset of organelles, usually ≥60% of the mtDNA copies need to contain deletions before any significant biochemical defect would be apparent.…”

Section: Effect Of Freezing and Thawing In Assisted Reproductive Techmentioning

confidence: 99%

Theory about the Embryo Cryo‐Treatment

Vladimirov

Tacheva

Dı́ez

2017

Reprod Medicine & Biology

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BackgroundTo create hypothesis, which can give a logical explanation related to the benefits of freezing/thawing embryos. Cryopreservation is not only a technology used for storing embryos, but also a method of embryo treatment that can potentially improve the success rate in infertile couples.MethodsFrom the analysis of multiple results in assisted reproductive technology, which have no satisfactory explanation to date, we found evidence to support a ‘therapeutic’ effect of the freezing/thawing of embryos on the process of recovery of the embryo and its subsequent implantation.ResultsFreezing/thawing is a way to activate the endogenous survival and repair responses in preimplantation embryos. Several molecular mechanisms can explain the higher success rate of ET using thawed embryos compared to fresh ET in women of advanced reproductive age, the higher miscarriage rate in cases of thawed blastocyst ET compared to thawed ET at early cleavage embryo, and the higher perinatal parameters of born children after thawed ET. Embryo thawing induces a stress. Controlled stress is not necessarily detrimental, because it generates a phenomenon that is counteracted by several known biological responses aimed to repair mitochondrial damage of membrane and protein misfolding. The term for favorable biological responses to low exposures to stress is called hormesis.ConclusionsThis thesis will summarize the role of cryopreservation in the activation of a hormetic response, preserving the mitochondrial function, improving survival, and having an impact on the process of implantation, miscarriage, and the development of pregnancy.

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The Role of Mitochondrial DNA Copy Number in Mammalian Fertility1

Cited by 366 publications

References 77 publications

A putative role for anti-Müllerian hormone (AMH) in optimising ovarian reserve expenditure

A putative role for anti-Müllerian hormone (AMH) in optimising ovarian reserve expenditure

Does serum cause lipid-droplet accumulation in bovine embryos produced in vitro, during developmental days 1 to 4?

Theory about the Embryo Cryo‐Treatment

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