The use of amplified cDNA to investigate the expression of seven imprinted genes in human oocytes and preimplantation embryos

doi:10.1093/molehr/7.9.839

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Molecular Human Reproduction, Vol. 7, No. 9, 839-844, September 2001
© 2001 European Society of Human Reproduction and Embryology

Embryology

The use of amplified cDNA to investigate the expression of seven imprinted genes in human oocytes and preimplantation embryos

Ashreena Salpekar¹, John Huntriss¹^,3, Virginia Bolton² and Marilyn Monk¹^,4

¹ Molecular Embryology Unit, Institute of Child Health, 30 Guilford Street, London WC1N 1EH and ² Assisted Conception Unit, Department of Obstetrics and Gynaecology, King's College School of Medicine and Dentistry, Denmark Hill, London SE5 8RX, UK

Abstract

Imprinted genes are characterized by expression of only oneof the two alleles according to its inheritance from the motheror the father. This mono-allelic expression must arise fromprimary differential epigenetic modification of the parentalalleles of the imprinted gene in the spermatozoon and the oocyte.Most of the information on the onset of imprinted gene expression,and on the molecular mechanisms regulating mono-allelic expression,have been derived from studies in the mouse. In this paper,we investigate the expression of seven imprinted genes in humanpreimplantation development. Due to limitations imposed by therarity of human embryos available for research, our approachhas been to screen amplified cDNA preparations prepared fromhuman unfertilized oocytes and individual embryos at each ofthe 4-cell, 8-cell and blastocyst stages. Gene-specific primerswere used to investigate expression of the imprinted genes bypolymerase chain reaction (PCR) analysis of these amplifiedcDNA. We found that expression is inherently variable in theamplified cDNA from embryo to embryo but the use of severalsamples at each stage showed that the SNRPN, UBE3A and PEG1genes are expressed throughout human preimplantation development.This was confirmed by direct analysis by gene-specific reversetranscription–PCR on a limited number of lysed embryos(one gene analysed per embryo). Thus, the amplified cDNA maybe used to rapidly identify those imprinted genes expressedin preimplantation development and, hence, those genes amenableto investigation of the epigenetic mechanisms regulating mono-allelicexpression. Confirmation of preimplantation expression alsoidentifies those imprinted diseases amenable to preimplantationdiagnosis, and the imprinted genes which may be used in assessmentof possible perturbations of imprinting following new proceduresin assisted reproduction. Our series of single embryo amplifiedcDNA are established as a valuable resource for comparativestudies of gene expression within one embryo and between embryosthroughout early human development. The amplified cDNA thuscircumvent the need for a continuous supply of human embryosfor studies on embryonic gene expression.

embryonic cDNA/genomic imprinting/human embryonic development/imprinted gene expression

Notes

³ Present address: Division of Obstetrics and Gynaecology, D Floor,Leeds General Infirmary, Belmont Grove, Leeds LS2 9NS, UK

⁴ To whom correspondence should be addressed. E-mail: mmonk{at}ich.ucl.ac.uk

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