Identifying novel regulatory effects for clinically relevant genes through the study of the Greek population

Author:

Rouskas Konstantinos1,Katsareli Efthymia A2,Amerikanou Charalampia2,Dimopoulos Alexandros C3,Glentis Stavros1,Kalantzi Alexandra1,Skoulakis Anargyros1,Panousis Nikolaos4,Ongen Halit5,Bielser Deborah5,Planchon Alexandra5,Romano Luciana5,Harokopos Vaggelis1,Reczko Martin3,Moulos Panagiotis3,Griniatsos Ioannis6,Diamantis Theodoros6,Dermitzakis Emmanouil T5,Ragoussis Jiannis7,Dedoussis George2,Dimas Antigone S1

Affiliation:

1. Institute for Bioinnovation, Biomedical Sciences Research Center 'Alexander Fleming', Vari, Greece

2. Department of Nutrition and Dietetics, School of Health Science and Education, Harokopio University, Athens, Greece

3. Institute for Fundamental Biomedical Science, Biomedical Sciences Research Center 'Alexander Fleming', Vari, Greece

4. Wellcome Sanger Institute, Hinxton, UK

5. Department of Genetic Medicine and Development, University of Geneva Medical School, Geneva, Switzerland

6. First Department of Surgery, National and Kapodistrian University of Athens, Medical School, Laiko Hospital, Athens, Greece

7. Department of Human Genetics, McGill University Genome Centre, McGill University, Montréal, QC, Canada

Abstract

Abstract Background Expression quantitative trait loci (eQTL) studies provide insights into regulatory mechanisms underlying disease risk. Expanding studies of gene regulation to underexplored populations and to medically relevant tissues offers potential to reveal yet unknown regulatory variants and to better understand disease mechanisms. Here, we performed eQTL mapping in subcutaneous (S) and visceral (V) adipose tissue from 106 Greek individuals (Greek Metabolic study, GM) and compared our findings to those from the Genotype-Tissue Expression (GTEx) resource. Results We identified 1,930 and 1,515 eGenes in S and V respectively, over 13% of which are not observed in GTEx adipose tissue, and that do not arise due to different ancestry. We report additional context-specific regulatory effects in genes of clinical interest (e.g. oncogene ST7) and in genes regulating responses to environmental stimuli (e.g. MIR21, SNX33). We suggest that a fraction of the reported differences across populations is due to environmental effects on gene expression, driving context-specific eQTLs, and suggest that environmental effects can determine the penetrance of disease variants thus shaping disease risk. We report that over half of GM eQTLs colocalize with GWAS SNPs and of these colocalizations 41% are not detected in GTEx. We also highlight the clinical relevance of S adipose tissue by revealing that inflammatory processes are upregulated in obese individuals, not only in V, but also in S tissue. Conclusions By focusing on an understudied population, our results provide further candidate genes for investigation regarding their role in adipose tissue biology and their contribution to disease risk and pathogenesis.

Funder

H2020 Marie Skłodowska-Curie Actions

European Molecular Biology Organization

General Secretariat for Research and Technology

Publisher

Research Square Platform LLC

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