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PAYWALLED__Association of epigenetic age and p16 INK4a with markers of T cell composition in a healthy cohort

aging biomarker senescence t-cell horvath clock cmv

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#1 Engadin

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Posted 05 May 2020 - 12:50 PM


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Abstract

How the measurement of aging biomarkers in peripheral blood T-lymphocytes (PBTLs) is influenced by cell composition is unclear. Here, we collected peripheral blood and isolated CD3+ PBTLs from 117 healthy couples between the ages of 21 and 72. Each sample was profiled for Horvath epigenetic clock (DNAm), p16INK4a expression, cytomegalovirus (CMV) seropositivity and 74 mRNA markers of PBTL subtype, differentiation, immune checkpoints and cytokine production.

 

Correlations between individual aging biomarkers (DNAm or p16INK4a) and PBTL mRNAs were corrected for chronologic age, sex and couple. DNAm measurements correlated with CMV seropositivity as well as PBTL mRNAs indicative of effector function (CD8AEOMESTBX21, GZMB), poor proliferative capacity (KLRG1, CD57), differentiation (CD45RO, CD45RA) and immune checkpoints (PDCD1TIGIT, LAG3CD160CD244).

 

By contrast, only three PBTL mRNAs: CD28CD244 and p14ARF, showed a significant association with p16INK4ap16INK4a expression also showed a weaker association with immunosenescent PBTL subsets than DNAm in flow cytometry analyses. These data suggest that PBTL composition has a greater influence on DNAm than p16INK4a and link accelerated epigenetic aging to immunosenescent phenotypes.

 

 

 

 

 

 

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Also tagged with one or more of these keywords: aging biomarker, senescence, t-cell, horvath clock, cmv

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