Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability

Genomic imprinting is important for normal brain development and aberrant imprinting has been associated with impaired cognition. We studied the imprinting status in selected imprints (H19, IGF2, SNRPN, PEG3, MEST1, NESPAS, KvDMR, IG-DMR and ZAC1) by pyrosequencing in blood samples from longitudinal...

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Autores principales: Lorgen-Ritchie, Marlene, Murray, Alison D., Ferguson-Smith, Anne C., Richards, Marcus, Horgan, Graham W., Phillips, Louise H., Hoad, Gwen, Gall, Ishbel, Harrison, Kristina, McNeill, Geraldine, Ito, Mitsuteru, Haggarty, Paul
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6358095/
https://www.ncbi.nlm.nih.gov/pubmed/30707743
http://dx.doi.org/10.1371/journal.pone.0211799
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author Lorgen-Ritchie, Marlene
Murray, Alison D.
Ferguson-Smith, Anne C.
Richards, Marcus
Horgan, Graham W.
Phillips, Louise H.
Hoad, Gwen
Gall, Ishbel
Harrison, Kristina
McNeill, Geraldine
Ito, Mitsuteru
Haggarty, Paul
author_facet Lorgen-Ritchie, Marlene
Murray, Alison D.
Ferguson-Smith, Anne C.
Richards, Marcus
Horgan, Graham W.
Phillips, Louise H.
Hoad, Gwen
Gall, Ishbel
Harrison, Kristina
McNeill, Geraldine
Ito, Mitsuteru
Haggarty, Paul
author_sort Lorgen-Ritchie, Marlene
collection PubMed
description Genomic imprinting is important for normal brain development and aberrant imprinting has been associated with impaired cognition. We studied the imprinting status in selected imprints (H19, IGF2, SNRPN, PEG3, MEST1, NESPAS, KvDMR, IG-DMR and ZAC1) by pyrosequencing in blood samples from longitudinal cohorts born in 1936 (n = 485) and 1921 (n = 223), and anterior hippocampus, posterior hippocampus, periventricular white matter, and thalamus from brains donated to the Aberdeen Brain Bank (n = 4). MEST1 imprint methylation was related to childhood cognitive ability score (-0.416 95% CI -0.792,-0.041; p = 0.030), with the strongest effect evident in males (-0.929 95% CI -1.531,-0.326; p = 0.003). SNRPN imprint methylation was also related to childhood cognitive ability (+0.335 95%CI 0.008,0.663; p = 0.045). A significant association was also observed for SNRPN methylation and adult crystallised cognitive ability (+0.262 95%CI 0.007,0.517; p = 0.044). Further testing of significant findings in a second cohort from the same region, but born in 1921, resulted in similar effect sizes and greater significance when the cohorts were combined (MEST1; -0.371 95% CI -0.677,-0.065; p = 0.017; SNRPN; +0.361 95% CI 0.079,0.643; p = 0.012). For SNRPN and MEST1 and four other imprints the methylation levels in blood and in the five brain regions were similar. Methylation of the paternally expressed, maternally methylated genes SNRPN and MEST1 in adult blood was associated with cognitive ability in childhood. This is consistent with the known importance of the SNRPN containing 15q11-q13 and the MEST1 containing 7q31-34 regions in cognitive function. These findings, and their sex specific nature in MEST1, point to new mechanisms through which complex phenotypes such as cognitive ability may be inherited. These mechanisms are potentially relevant to both the heritable and non-heritable components of cognitive ability. The process of epigenetic imprinting—within SNRPN and MEST1 in particular—and the factors that influence it, are worthy of further study in relation to the determinants of cognitive ability.
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spelling pubmed-63580952019-02-15 Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability Lorgen-Ritchie, Marlene Murray, Alison D. Ferguson-Smith, Anne C. Richards, Marcus Horgan, Graham W. Phillips, Louise H. Hoad, Gwen Gall, Ishbel Harrison, Kristina McNeill, Geraldine Ito, Mitsuteru Haggarty, Paul PLoS One Research Article Genomic imprinting is important for normal brain development and aberrant imprinting has been associated with impaired cognition. We studied the imprinting status in selected imprints (H19, IGF2, SNRPN, PEG3, MEST1, NESPAS, KvDMR, IG-DMR and ZAC1) by pyrosequencing in blood samples from longitudinal cohorts born in 1936 (n = 485) and 1921 (n = 223), and anterior hippocampus, posterior hippocampus, periventricular white matter, and thalamus from brains donated to the Aberdeen Brain Bank (n = 4). MEST1 imprint methylation was related to childhood cognitive ability score (-0.416 95% CI -0.792,-0.041; p = 0.030), with the strongest effect evident in males (-0.929 95% CI -1.531,-0.326; p = 0.003). SNRPN imprint methylation was also related to childhood cognitive ability (+0.335 95%CI 0.008,0.663; p = 0.045). A significant association was also observed for SNRPN methylation and adult crystallised cognitive ability (+0.262 95%CI 0.007,0.517; p = 0.044). Further testing of significant findings in a second cohort from the same region, but born in 1921, resulted in similar effect sizes and greater significance when the cohorts were combined (MEST1; -0.371 95% CI -0.677,-0.065; p = 0.017; SNRPN; +0.361 95% CI 0.079,0.643; p = 0.012). For SNRPN and MEST1 and four other imprints the methylation levels in blood and in the five brain regions were similar. Methylation of the paternally expressed, maternally methylated genes SNRPN and MEST1 in adult blood was associated with cognitive ability in childhood. This is consistent with the known importance of the SNRPN containing 15q11-q13 and the MEST1 containing 7q31-34 regions in cognitive function. These findings, and their sex specific nature in MEST1, point to new mechanisms through which complex phenotypes such as cognitive ability may be inherited. These mechanisms are potentially relevant to both the heritable and non-heritable components of cognitive ability. The process of epigenetic imprinting—within SNRPN and MEST1 in particular—and the factors that influence it, are worthy of further study in relation to the determinants of cognitive ability. Public Library of Science 2019-02-01 /pmc/articles/PMC6358095/ /pubmed/30707743 http://dx.doi.org/10.1371/journal.pone.0211799 Text en © 2019 Lorgen-Ritchie et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Lorgen-Ritchie, Marlene
Murray, Alison D.
Ferguson-Smith, Anne C.
Richards, Marcus
Horgan, Graham W.
Phillips, Louise H.
Hoad, Gwen
Gall, Ishbel
Harrison, Kristina
McNeill, Geraldine
Ito, Mitsuteru
Haggarty, Paul
Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability
title Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability
title_full Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability
title_fullStr Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability
title_full_unstemmed Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability
title_short Imprinting methylation in SNRPN and MEST1 in adult blood predicts cognitive ability
title_sort imprinting methylation in snrpn and mest1 in adult blood predicts cognitive ability
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6358095/
https://www.ncbi.nlm.nih.gov/pubmed/30707743
http://dx.doi.org/10.1371/journal.pone.0211799
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