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A global disorder of imprinting in the human female germ line

Author

Listed:
  • Hannah Judson

    (University of Leeds, Molecular Medicine Unit, St. James's University Hospital)

  • Bruce E. Hayward

    (University of Leeds, Molecular Medicine Unit, St. James's University Hospital)

  • Eamonn Sheridan

    (University of Leeds, Molecular Medicine Unit, St. James's University Hospital)

  • David T. Bonthron

    (University of Leeds, Molecular Medicine Unit, St. James's University Hospital)

Abstract

Imprinted genes are expressed differently depending on whether they are carried by a chromosome of maternal or paternal origin. Correct imprinting is established by germline-specific modifications; failure of this process underlies several inherited human syndromes1,2,3,4,5. All these imprinting control defects are cis-acting, disrupting establishment or maintenance of allele-specific epigenetic modifications across one contiguous segment of the genome. In contrast, we report here an inherited global imprinting defect. This recessive maternal-effect mutation disrupts the specification of imprints at multiple, non-contiguous loci, with the result that genes normally carrying a maternal methylation imprint assume a paternal epigenetic pattern on the maternal allele. The resulting conception is phenotypically indistinguishable from an androgenetic complete hydatidiform mole6, in which abnormal extra-embryonic tissue proliferates while development of the embryo is absent or nearly so. This disorder offers a genetic route to the identification of trans-acting oocyte factors that mediate maternal imprint establishment.

Suggested Citation

  • Hannah Judson & Bruce E. Hayward & Eamonn Sheridan & David T. Bonthron, 2002. "A global disorder of imprinting in the human female germ line," Nature, Nature, vol. 416(6880), pages 539-542, April.
  • Handle: RePEc:nat:nature:v:416:y:2002:i:6880:d:10.1038_416539a
    DOI: 10.1038/416539a
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