Using Mouse Oocytes to Assess Human Gene Function During Meiosis I

Overview

Journal J Vis Exp

Specialties Biology
General Medicine

Date 2018 May 1

PMID 29708548

Citations 2

Authors

Diego Marin

Alexandra L Nguyen

Richard T Scott Jr

Karen Schindler

Affiliations

Soon will be listed here.

Abstract

Embryonic aneuploidy is the major genetic cause of infertility in humans. Most of these events originate during female meiosis, and albeit positively correlated with maternal age, age alone is not always predictive of the risk of generating an aneuploid embryo. Therefore, gene variants might account for incorrect chromosome segregation during oogenesis. Given that access to human oocytes is limited for research purposes, a series of assays were developed to study human gene function during meiosis I using mouse oocytes. First, messenger RNA (mRNA) of the gene and gene variant of interest are microinjected into prophase I-arrested mouse oocytes. After allowing time for expression, oocytes are synchronously released into meiotic maturation to complete meiosis I. By tagging the mRNA with a sequence of a fluorescent reporter, such as green fluorescent protein (Gfp), the localization of the human protein can be assessed in addition to the phenotypic alterations. For example, gain or loss of function can be investigated by establishing experimental conditions that challenge the gene product to fix meiotic errors. Although this system is advantageous in investigating human protein function during oogenesis, adequate interpretation of results should be undertaken given that protein expression is not at endogenous levels and, unless controlled for (i.e. knocked out or down), murine homologs are also present in the system.

Citing Articles

Evaluation of the Spindle Assembly Checkpoint Integrity in Mouse Oocytes.

Aboelenain M, Schindler K, Blengini C J Vis Exp. 2022; (187).

PMID: 36190266 PMC: 10314320. DOI: 10.3791/64459.

Genetic Interactions between the Aurora Kinases Reveal New Requirements for AURKB and AURKC during Oocyte Meiosis.

Nguyen A, Drutovic D, Vazquez B, El Yakoubi W, Gentilello A, Malumbres M Curr Biol. 2018; 28(21):3458-3468.e5.

PMID: 30415701 PMC: 6234855. DOI: 10.1016/j.cub.2018.08.052.

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