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The Histone Modification H3K4me3 is Altered at the <i>ANK1</i> Locus in Alzheimer's Disease Brain

Adam R. Smith, Rebecca G. Smith, Ruby I. MacDonald, Sarah J. Marzi, Joe Burrage, Claire Troakes, Safa Al‐Sarraj, Jonathan Mill, Katie Lunnon

2021Future Science OA23 citationsDOIOpen Access PDF

Abstract

Several epigenome-wide association studies of DNA methylation have highlighted altered DNA methylation in the ANK1 gene in Alzheimer's disease (AD) brain samples. However, no study has specifically examined ANK1 histone modifications in the disease. We use chromatin immunoprecipitation-qPCR to quantify tri-methylation at histone 3 lysine 4 (H3K4me3) and 27 (H3K27me3) in the ANK1 gene in entorhinal cortex from donors with high (n = 59) or low (n = 29) Alzheimer's disease pathology. We demonstrate decreased levels of H3K4me3, a marker of active gene transcription, with no change in H3K27me3, a marker of inactive genes. H3K4me3 is negatively correlated with DNA methylation in specific regions of the ANK1 gene. Our study suggests that the ANK1 gene shows altered epigenetic marks indicative of reduced gene activation in Alzheimer's disease.

Topics & Concepts

DNA methylationH3K4me3EpigeneticsBiologyHistoneEpigenomeHistone methylationGeneticsChromatin immunoprecipitationEpigenomicsRegulation of gene expressionPromoterGene expressionGeneEpigenetics and DNA MethylationGenetics and Neurodevelopmental DisordersGenetic Syndromes and Imprinting
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