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Alterations in oocyte mitochondrial number and function are related to spindle defects and occur with maternal aging in mice and humans

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TLDR
Oocytes of older females are more susceptible to perturbations in mitochondrial number and function, which are associated with increased spindle abnormalities and oxidative stress during in vitro maturation, demonstrating that oocyte mitochondria play a critical role in age-related infertility.
Abstract
The objective of this work was to determine the role of mitochondria in the loss of oocyte quality with maternal aging. Our results show that mitochondrial DNA (mtDNA) copy number and function are reduced in eggs from aged mice after both in vivo and in vitro maturation. Higher incidences of spindle abnormalities were observed in old eggs. However, no correlation with egg ATP content was found. In vitro matured eggs from aged mice did not have a normal cortical distribution of active mitochondria and were subject to increased oxidative stress due to higher levels of reactive oxygen species and lower expression of glutamate-cysteine ligase, catalytic subunit (Gclc). Supplementation of antioxidants during in vitro maturation of old eggs mitigated this affect, resulting in increased mtDNA copy number and mitochondrial function, a mitochondria distribution pattern similar to young eggs, and improved chromosomal alignment. Eggs from women of advanced maternal age (AMA) had lower mitochondrial function than eggs from young women, although both age groups displayed a cortical distribution pattern of active mitochondria. In contrast to the mouse, human eggs from AMA women had higher mtDNA copy number than eggs from young women following in vitro maturation. In summary, oocytes of older females are more susceptible to perturbations in mitochondrial number and function, which are associated with increased spindle abnormalities and oxidative stress during in vitro maturation. These results demonstrate that oocyte mitochondria play a critical role in age-related infertility.

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Journal ArticleDOI

Impact of Oxidative Stress on Age-Associated Decline in Oocyte Developmental Competence.

TL;DR: Increased ROS and increased vulnerability of oocytes to ROS lead to spindle instability, chromosomal abnormalities, telomere shortening, and reduced developmental competence of aged oocytes, focusing on oxidative stress (OS) in oocytes.
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Impact of oxidative stress on male and female germ cells: implications for fertility

TL;DR: Male and female germ lines are vulnerable to oxidative stress and antioxidants should have some role to play in the preservation of reproductive function in both men and women; however, it still await appropriate trials to test this hypothesis.
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The Role of Oxidative Stress and Natural Antioxidants in Ovarian Aging.

TL;DR: It is shown that oxidative stress plays a role in the etiology of ovarian aging and promotes the development of other ovarian aging-related etiologies, including telomere shortening, mitochondrial dysfunction, apoptosis, and inflammation, which raises the prospect of oxidative stress modulator-natural antioxidants as therapeutic interventions for delaying ovarian aging.
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The spatio-temporal dynamics of mitochondrial membrane potential during oocyte maturation.

TL;DR: A new approach to reliably measure ΔΨm is provided that has shed new light onto the spatio-temporal regulation of mitochondrial function in oocytes and early embryos and suggests that mitochondrial activity is adaptive and responsive to the events of oocyte maturation at both a global and local level.
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The Role of Resveratrol in Mammalian Reproduction

TL;DR: In males, resveratrol enhances testes function and spermatogenesis through activation of the AMPK pathway and has been supplemented to semen extenders, improving the preservation of sperm quality.
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Consequences of bovine oocyte maturation, fertilization or early embryo development in vitro versus in vivo: implications for blastocyst yield and blastocyst quality.

TL;DR: The results indicate that the intrinsic quality of the oocyte is the main factor affecting blastocyst yields, while the conditions of embryo culture have a crucial role in determining Blastocyst quality.
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