Epigenomic Signature of Adrenoleukodystrophy Predicts Compromised Oligodendrocyte Differentiation

Overview

Journal Brain Pathol

Date 2018 Feb 25

PMID 29476661

Citations 13

Authors

Agatha Schluter

Juan Sandoval

Stephane Fourcade

Angel Diaz-Lagares

Montserrat Ruiz

Patrizia Casaccia

Manel Esteller

Aurora Pujol

Affiliations

Soon will be listed here.

Abstract

Epigenomic changes may either cause disease or modulate its expressivity, adding a layer of complexity to mendelian diseases. X-linked adrenoleukodystrophy (X-ALD) is a rare neurometabolic condition exhibiting discordant phenotypes, ranging from a childhood cerebral inflammatory demyelination (cALD) to an adult-onset mild axonopathy in spinal cords (AMN). The AMN form may occur with superimposed inflammatory brain demyelination (cAMN). All patients harbor loss of function mutations in the ABCD1 peroxisomal transporter of very-long chain fatty acids. The factors that account for the lack of genotype-phenotype correlation, even within the same family, remain largely unknown. To gain insight into this matter, here we compared the genome-wide DNA methylation profiles of morphologically intact frontal white matter areas of children affected by cALD with adult cAMN patients, including male controls in the same age group. We identified a common methylomic signature between the two phenotypes, comprising (i) hypermethylation of genes harboring the H3K27me3 mark at promoter regions, (ii) hypermethylation of genes with major roles in oligodendrocyte differentiation such as MBP, CNP, MOG and PLP1 and (iii) hypomethylation of immune-associated genes such as IFITM1 and CD59. Moreover, we found increased hypermethylation in CpGs of genes involved in oligodendrocyte differentiation, and also in genes with H3K27me3 marks in their promoter regions in cALD compared with cAMN, correlating with transcriptional and translational changes. Further, using a penalized logistic regression model, we identified the combined methylation levels of SPG20, UNC45A and COL9A3 and also, the combined expression levels of ID4 and MYRF to be good markers capable of discriminating childhood from adult inflammatory phenotypes. We thus propose the hypothesis that an epigenetically controlled, altered transcriptional program may drive an impaired oligodendrocyte differentiation and aberrant immune activation in X-ALD patients. These results shed light into disease pathomechanisms and uncover putative biomarkers of interest for prognosis and phenotypic stratification.

Citing Articles

Pathophysiology of X-Linked Adrenoleukodystrophy: Updates on Molecular Mechanisms.

Parasar P, Kaur N, Singh J J Biotechnol Biomed. 2024; 7(2):277-288.

PMID: 39056013 PMC: 11271253. DOI: 10.26502/jbb.2642-91280151.

The pathology of X-linked adrenoleukodystrophy: tissue specific changes as a clue to pathophysiology.

Yska H, Engelen M, Bugiani M Orphanet J Rare Dis. 2024; 19(1):138.

PMID: 38549180 PMC: 10976706. DOI: 10.1186/s13023-024-03105-0.

IPSC-Derived Astrocytes to Model Neuroinflammatory and Metabolic Responses in X-linked Adrenoleukodystrophy.

Parasar P, Kaur N, Singh J J Biotechnol Biomed. 2023; 6(3):281-293.

PMID: 38077449 PMC: 10705002. DOI: 10.26502/jbb.2642-91280091.

Adrenomyeloneuropathy with Later Development of Cerebral Form Caused by a Hemizygous Splice-site Variant in ABCD1.

Takegami N, Matsukawa T, Hamada M, Tanifuji S, Tamura T, Yamaguchi-Takegami N Intern Med. 2023; 63(7):999-1004.

PMID: 37558478 PMC: 11045382. DOI: 10.2169/internalmedicine.2240-23.

The stability of the myelinating oligodendrocyte transcriptome is regulated by the nuclear lamina.

Pruvost M, Patzig J, Yattah C, Selcen I, Hernandez M, Park H Cell Rep. 2023; 42(8):112848.

PMID: 37515770 PMC: 10600948. DOI: 10.1016/j.celrep.2023.112848.

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