Meiosis in oocytes: predisposition to aneuploidy and its increased incidence with age

Keith T. Jones¹

Institute for Cell and Molecular Biosciences, The Medical School, University of Newcastle, Framlington Place, Newcastle, NE2 4HH, UK

To whom correspondence should be addressed at: ¹ Correspondence address. Tel: +44-191-222-6963; Fax: +44-191-222-7424; k.t.jones{at}ncl.ac.uk

Mammalian oocytes begin meiosis in the fetal ovary, but onlycomplete it when fertilized in the adult reproductive tract.This review examines the cell biology of this protracted process:from entry of primordial germ cells into meiosis to conception.The defining feature of meiosis is two consecutive cell divisions(meiosis I and II) and two cell cycle arrests: at the germinalvesicle (GV), dictyate stage of prophase I and at metaphaseII. These arrests are spanned by three key events, the focusof this review: (i) passage from mitosis to GV arrest duringfetal life, regulated by retinoic acid; (ii) passage throughmeiosis I and (iii) completion of meiosis II following fertilization,both meiotic divisions being regulated by cyclin-dependent kinase(CDK1) activity. Meiosis I in human oocytes is associated withan age-related high rate of chromosomal mis-segregation, suchas trisomy 21 (Down’s syndrome), resulting in aneuploidconceptuses. Although aneuploidy is likely to be multifactorial,oocytes from older women may be predisposed to be becoming aneuploidas a consequence of an age-long decline in the cohesive tiesholding chromosomes together. Such loss goes undetected by theoocyte during meiosis I either because its ability to respondand block division also deteriorates with age, or as a consequenceof being inherently unable to respond to the types of segregationdefects induced by cohesion loss.

Key words: aneuploidy / fertilization / meiosis / cocyte

Received on September 18, 2007; revised October 19, 2007; accepted on November 2, 2007

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Meiosis in oocytes: predisposition to aneuploidy and its increased incidence with age