4.6 Article

Unraveling the Regulatory Mechanisms Underlying Tissue-Dependent Genetic Variation of Gene Expression

Journal

PLOS GENETICS
Volume 8, Issue 1, Pages -

Publisher

PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pgen.1002431

Keywords

-

Funding

  1. IOP [IGE05012A]
  2. Netherlands Organisation for Scientific Research (NWO) VICI [918.66.620]
  3. European Union [201379]
  4. Dutch Diabetes Foundation [2006.00.007]
  5. Wellcome Trust [084743]
  6. Medical Research Council UK [G1001158]
  7. Juvenile Diabetes Research Foundation [33-2008-402]
  8. NWO VENI [863.09.007, 916.10.135]
  9. Netherlands Genomics Initiative [92519031]
  10. NWO [90.700.281]
  11. Thierry Latran Foundation
  12. Transnational University Limburg
  13. European Community [259867]
  14. Medical Research Council [G1001158] Funding Source: researchfish
  15. MRC [G1001158] Funding Source: UKRI

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It is known that genetic variants can affect gene expression, but it is not yet completely clear through what mechanisms genetic variation mediate this expression. We therefore compared the cis-effect of single nucleotide polymorphisms (SNPs) on gene expression between blood samples from 1,240 human subjects and four primary non-blood tissues (liver, subcutaneous, and visceral adipose tissue and skeletal muscle) from 85 subjects. We characterized four different mechanisms for 2,072 probes that show tissue-dependent genetic regulation between blood and non-blood tissues: on average 33.2% only showed cis-regulation in non-blood tissues; 14.5% of the eQTL probes were regulated by different, independent SNPs depending on the tissue of investigation. 47.9% showed a different effect size although they were regulated by the same SNPs. Surprisingly, we observed that 4.4% were regulated by the same SNP but with opposite allelic direction. We show here that SNPs that are located in transcriptional regulatory elements are enriched for tissue-dependent regulation, including SNPs at 3' and 5' untranslated regions (P=1.84x10(-5) and 4.7x10(-4), respectively) and SNPs that are synonymous-coding (P = 9.9x10(-4)). SNPs that are associated with complex traits more often exert a tissue-dependent effect on gene expression (P = 2.6x10(-10)). Our study yields new insights into the genetic basis of tissue-dependent expression and suggests that complex trait associated genetic variants have even more complex regulatory effects than previously anticipated.

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