Large-scale Methylation Analysis of Human Genomic DNA Reveals Tissue-specific Differences Between the Methylation Profiles of Genes and Pseudogenes

Overview

Journal Hum Mol Genet

Specialties Genetics
Molecular Biology

Date 2000 Nov 7

PMID 11063724

Citations 44

Authors

C Grunau

W Hindermann

A Rosenthal

Affiliations

Soon will be listed here.

Abstract

Cytosine in CpG dinucleotides is frequently found to be methylated in the DNA of higher eukaryotes and differential methylation has been proposed to be a key element in the organization of gene expression in man. To address this question systematically, we used bisulfite genomic sequencing to study the methylation patterns of three X-linked genes and one autosomal pseudogene in two adult individuals and across nine different tissues. Two of the genes, SLC6A8 and MSSK1, are tissue-specifically expressed. CDM is expressed ubiquitously. The pseudogene, psi SLC6A8, is exclusively expressed in the testis. The promoter regions of the SLC6A8, MSSK1 and CDM genes were found to be essentially unmethylated in all tissues, regardless of their relative expression level. In contrast, the pseudogene psi SLC6A8 shows high methylation of the CpG islands in all somatic tissues but complete demethylation in testis. Methylation profiles in different tissues are similar in shape but not identical. The data for the two investigated individuals suggest that methylation profiles of individual genes are tissue specific. Taken together, our findings support a model in which the bodies of the genes are predominantly methylated and thus insulated from the interaction with DNA-binding proteins. Only unmethylated promoter regions are accessible for binding and interaction. Based on this model we propose to use DNA methylation studies in conjunction with large-scale sequencing approaches as a tool for the prediction of cis-acting genomic regions, for the identification of cryptic and potentially active CpG islands and for the preliminary distinction of genes and pseudogenes.

Citing Articles

In search of epigenetic hallmarks of different tissues: an integrative omics study of horse liver, lung, and heart.

Semik-Gurgul E, Pawlina-Tyszko K, Gurgul A, Szmatola T, Rybinska J, Zabek T Mamm Genome. 2024; 35(4):600-620.

PMID: 39143382 PMC: 11522055. DOI: 10.1007/s00335-024-10057-0.

Functions of SRPK, CLK and DYRK kinases in stem cells, development, and human developmental disorders.

Hogg E, Findlay G FEBS Lett. 2023; 597(19):2375-2415.

PMID: 37607329 PMC: 10952393. DOI: 10.1002/1873-3468.14723.

Genetic analysis of DNA methylation in dyslipidemia: a case-control study.

Liu S, Li Y, Wei X, Adi D, Wang Y, Han M PeerJ. 2022; 10:e14590.

PMID: 36570009 PMC: 9774006. DOI: 10.7717/peerj.14590.

Pseudogenes and Liquid Phase Separation in Epigenetic Expression.

Nsengimana B, Khan F, Awan U, Wang D, Fang N, Wei W Front Oncol. 2022; 12:912282.

PMID: 35875144 PMC: 9305658. DOI: 10.3389/fonc.2022.912282.

In Response to Abiotic Stress, DNA Methylation Confers EpiGenetic Changes in Plants.

Akhter Z, Bi Z, Ali K, Sun C, Fiaz S, Haider F Plants (Basel). 2021; 10(6).

PMID: 34070712 PMC: 8227271. DOI: 10.3390/plants10061096.