Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and children

Abstract Background Age-related changes in adaptive and innate immune cells have been associated with a decline in effective immunity and chronic, low-grade inflammation. Epigenetic, transcriptional, and functional changes in monocytes occur with aging, though most studies to date have focused on di...

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Main Authors: Katherine R. Dobbs, Paula Embury, Emmily Koech, Sidney Ogolla, Stephen Munga, James W. Kazura, Arlene E. Dent
Format: Article
Language:English
Published: BMC 2021-03-01
Series:Immunity & Ageing
Subjects:
Online Access:https://doi.org/10.1186/s12979-021-00223-2
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spelling doaj-b5de2685d0b942f9b7fcbb23589b6e2c2021-03-11T12:56:34ZengBMCImmunity & Ageing1742-49332021-03-0118111410.1186/s12979-021-00223-2Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and childrenKatherine R. Dobbs0Paula Embury1Emmily Koech2Sidney Ogolla3Stephen Munga4James W. Kazura5Arlene E. Dent6Center for Global Health and Diseases, Case Western Reserve UniversityCenter for Global Health and Diseases, Case Western Reserve UniversityCentre for Global Health Research, Kenya Medical Research InstituteCentre for Global Health Research, Kenya Medical Research InstituteCentre for Global Health Research, Kenya Medical Research InstituteCenter for Global Health and Diseases, Case Western Reserve UniversityCenter for Global Health and Diseases, Case Western Reserve UniversityAbstract Background Age-related changes in adaptive and innate immune cells have been associated with a decline in effective immunity and chronic, low-grade inflammation. Epigenetic, transcriptional, and functional changes in monocytes occur with aging, though most studies to date have focused on differences between young adults and the elderly in populations with European ancestry; few data exist regarding changes that occur in circulating monocytes during the first few decades of life or in African populations. We analyzed DNA methylation profiles, cytokine production, and inflammatory gene expression profiles in monocytes from young adults and children from western Kenya. Results We identified several hypo- and hyper-methylated CpG sites in monocytes from Kenyan young adults vs. children that replicated findings in the current literature of differential DNA methylation in monocytes from elderly persons vs. young adults across diverse populations. Differentially methylated CpG sites were also noted in gene regions important to inflammation and innate immune responses. Monocytes from Kenyan young adults vs. children displayed increased production of IL-8, IL-10, and IL-12p70 in response to TLR4 and TLR2/1 stimulation as well as distinct inflammatory gene expression profiles. Conclusions These findings complement previous reports of age-related methylation changes in isolated monocytes and provide novel insights into the role of age-associated changes in innate immune functions.https://doi.org/10.1186/s12979-021-00223-2MonocyteDNA methylationEpigeneticAgeingAgingInnate immune
collection DOAJ
language English
format Article
sources DOAJ
author Katherine R. Dobbs
Paula Embury
Emmily Koech
Sidney Ogolla
Stephen Munga
James W. Kazura
Arlene E. Dent
spellingShingle Katherine R. Dobbs
Paula Embury
Emmily Koech
Sidney Ogolla
Stephen Munga
James W. Kazura
Arlene E. Dent
Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and children
Immunity & Ageing
Monocyte
DNA methylation
Epigenetic
Ageing
Aging
Innate immune
author_facet Katherine R. Dobbs
Paula Embury
Emmily Koech
Sidney Ogolla
Stephen Munga
James W. Kazura
Arlene E. Dent
author_sort Katherine R. Dobbs
title Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and children
title_short Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and children
title_full Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and children
title_fullStr Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and children
title_full_unstemmed Age-related differences in monocyte DNA methylation and immune function in healthy Kenyan adults and children
title_sort age-related differences in monocyte dna methylation and immune function in healthy kenyan adults and children
publisher BMC
series Immunity & Ageing
issn 1742-4933
publishDate 2021-03-01
description Abstract Background Age-related changes in adaptive and innate immune cells have been associated with a decline in effective immunity and chronic, low-grade inflammation. Epigenetic, transcriptional, and functional changes in monocytes occur with aging, though most studies to date have focused on differences between young adults and the elderly in populations with European ancestry; few data exist regarding changes that occur in circulating monocytes during the first few decades of life or in African populations. We analyzed DNA methylation profiles, cytokine production, and inflammatory gene expression profiles in monocytes from young adults and children from western Kenya. Results We identified several hypo- and hyper-methylated CpG sites in monocytes from Kenyan young adults vs. children that replicated findings in the current literature of differential DNA methylation in monocytes from elderly persons vs. young adults across diverse populations. Differentially methylated CpG sites were also noted in gene regions important to inflammation and innate immune responses. Monocytes from Kenyan young adults vs. children displayed increased production of IL-8, IL-10, and IL-12p70 in response to TLR4 and TLR2/1 stimulation as well as distinct inflammatory gene expression profiles. Conclusions These findings complement previous reports of age-related methylation changes in isolated monocytes and provide novel insights into the role of age-associated changes in innate immune functions.
topic Monocyte
DNA methylation
Epigenetic
Ageing
Aging
Innate immune
url https://doi.org/10.1186/s12979-021-00223-2
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