Testing two models describing how methylome-wide studies in blood are informative for psychiatric conditions

Author:

Aberg Karolina A1,Xie Lin Y2,McClay Joseph L2,Nerella Srilaxmi2,Vunck Sarah23,Snider Sarah23,Beardsley Patrick M23,van den Oord Edwin JCG2

Affiliation:

1. Center for Biomarker Research & Personalized Medicine, School of Pharmacy, Virginia Commonwealth University, 1112 East Clay Street, PO Box 980533, Richmond, VA 23298, USA. .

2. Center for Biomarker Research & Personalized Medicine, School of Pharmacy, Virginia Commonwealth University, 1112 East Clay Street, PO Box 980533, Richmond, VA 23298, USA

3. Department of Pharmacology & Toxicology, School of Medicine, Virginia Commonwealth University, PO Box 980613, Richmond, VA 23298, USA

Abstract

Aim: As the primary relevant tissue (brain) for psychiatric disorders is commonly not available, we aimed to investigate whether blood can be used as a proxy in methylation studies on the basis of two models. In the ‘signature’ model methylation–disease associations occur because a disease-causing factor affected methylation in the blood. In the ‘mirror-site’ model the methylation status in the blood is correlated with the corresponding disease-causing site in the brain. Materials, methods & results: Methyl-binding domain enrichment and next-generation sequencing of the blood, cortex and hippocampus from four haloperidol-treated and ten untreated C57BL/6 mice revealed high levels of correlation in methylation across tissues. Despite the treatment inducing a large number of methylation changes, this correlation remains high. Conclusion: Our results show that, consistent with the signature model, factors that affect brain processes (i.e., haloperidol) leave biomarker signatures in the blood and, consistent with the mirror-site model, the methylation status of many sites in the blood mirror those in the brain.

Publisher

Future Medicine Ltd

Subject

Cancer Research,Genetics

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