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Partial Loss of Genomic Imprinting Reveals Important Roles for Kcnq1 and Peg10 Imprinted Domains in Placental Development

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  • Erik Koppes
  • Katherine P Himes
  • J Richard Chaillet

Abstract

Mutations in imprinted genes or their imprint control regions (ICRs) produce changes in imprinted gene expression and distinct abnormalities in placental structure, indicating the importance of genomic imprinting to placental development. We have recently shown that a very broad spectrum of placental abnormalities associated with altered imprinted gene expression occurs in the absence of the oocyte–derived DNMT1o cytosine methyltransferase, which normally maintains parent-specific imprinted methylation during preimplantation. The absence of DNMT1o partially reduces inherited imprinted methylation while retaining the genetic integrity of imprinted genes and their ICRs. Using this novel system, we undertook a broad and inclusive approach to identifying key ICRs involved in placental development by correlating loss of imprinted DNA methylation with abnormal placental phenotypes in a mid-gestation window (E12.5-E15.5). To these ends we measured DNA CpG methylation at 15 imprinted gametic differentially methylated domains (gDMDs) that overlap known ICRs using EpiTYPER-mass array technology, and linked these epigenetic measurements to histomorphological defects. Methylation of some imprinted gDMDs, most notably Dlk1, was nearly normal in mid-gestation DNMT1o-deficient placentas, consistent with the notion that cells having lost methylation on these DMDs do not contribute significantly to placental development. Most imprinted gDMDs however showed a wide range of methylation loss among DNMT1o-deficient placentas. Two striking associations were observed. First, loss of DNA methylation at the Peg10 imprinted gDMD associated with decreased embryonic viability and decreased labyrinthine volume. Second, loss of methylation at the Kcnq1 imprinted gDMD was strongly associated with trophoblast giant cell (TGC) expansion. We conclude that the Peg10 and Kcnq1 ICRs are key regulators of mid-gestation placental function.

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  • Erik Koppes & Katherine P Himes & J Richard Chaillet, 2015. "Partial Loss of Genomic Imprinting Reveals Important Roles for Kcnq1 and Peg10 Imprinted Domains in Placental Development," PLOS ONE, Public Library of Science, vol. 10(8), pages 1-21, August.
    • Handle: RePEc:plo:pone00:0135202
    DOI: 10.1371/journal.pone.0135202
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    1. Miguel Constância & Myriam Hemberger & Jennifer Hughes & Wendy Dean & Anne Ferguson-Smith & Reinald Fundele & Francesca Stewart & Gavin Kelsey & Abigail Fowden & Colin Sibley & Wolf Reik, 2002. "Placental-specific IGF-II is a major modulator of placental and fetal growth," Nature, Nature, vol. 417(6892), pages 945-948, June.
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    Cited by:

    1. Lali Mwamaka Sharifu & Li jia qi & Feng Ling & Wang Shao shuai & Joyce Wanjiru Maingi & Paul Kibaba & Alfred Martin Omondi, 2020. "Imprinted Gene Regulation in the Placenta and Fetal Development," Biomedical Journal of Scientific & Technical Research, Biomedical Research Network+, LLC, vol. 28(3), pages 21560-21567, June.

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