Predicting Infertility: How Genetic Variants in Oocyte Spindle Genes Affect Egg Quality.

Adv Anat Embryol Cell Biol

Department of Genetics, Rutgers University, Piscataway, NJ, USA.

Published: July 2024

AI Article Synopsis

  • Successful reproduction depends on the combination of a chromosomally normal egg and sperm, with oocytes needing accurate chromosome segregation during meiosis.
  • The oocyte spindle, a critical structure for this chromosome segregation, can be affected by genetic variations in several spindle-associated proteins, impacting female fertility.
  • This chapter examines how specific genetic variants in proteins like TUBB8 and AURKA can lead to oocyte dysfunction and adverse fertility outcomes, such as maturation arrest and pregnancy loss.

Article Abstract

Successful reproduction relies on the union of a single chromosomally normal egg and sperm. Chromosomally normal eggs develop from precursor cells, called oocytes, that have undergone accurate chromosome segregation. The process of chromosome segregation is governed by the oocyte spindle, a unique cytoskeletal machine that splits chromatin content of the meiotically dividing oocyte. The oocyte spindle develops and functions in an idiosyncratic process, which is vulnerable to genetic variation in spindle-associated proteins. Human genetic variants in several spindle-associated proteins are associated with poor clinical fertility outcomes, suggesting that heritable etiologies for oocyte dysfunction leading to infertility exist and that the spindle is a crux for female fertility. This chapter examines the mammalian oocyte spindle through the lens of human genetic variation, covering the genes TUBB8, TACC3, CEP120, AURKA, AURKC, AURKB, BUB1B, and CDC20. Specifically, it explores how patient-identified variants perturb spindle development and function, and it links these molecular changes in the oocyte to their cognate clinical consequences, such as oocyte maturation arrest, elevated egg aneuploidy, primary ovarian insufficiency, and recurrent pregnancy loss. This discussion demonstrates that small genetic errors in oocyte meiosis can result in remarkably far-ranging embryonic consequences, and thus reveals the importance of the oocyte's fine machinery in sustaining life.

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Source
http://dx.doi.org/10.1007/978-3-031-55163-5_1DOI Listing

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