Scientific Reports (Jul 2017)

Common variants of T-cells contribute differently to phenotypic variation in sarcoidosis

  • Natalia V. Rivera,
  • Michael Hagemann-Jensen,
  • Manuel A. R. Ferreira,
  • Susanna Kullberg,
  • Anders Eklund,
  • Nicholas G. Martin,
  • Leonid Padyukov,
  • Johan Grunewald

DOI
https://doi.org/10.1038/s41598-017-05754-7
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 13

Abstract

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Abstract The involvement of the immune system, particularly the role of T-cells, in sarcoidosis is unclear. The existence of higher CD4+ T-cells and increased CD4/CD8 ratio may indicate a pathogenic role of T-cells in the disease. In this study, we quantified the contribution of T-cells associated variants and of CD4/CD8 ratio in sarcoidosis phenotypes, Löfgren’s syndrome (LS) and non- Löfgren’s syndrome (non-LS). We employed a polygenic-based approach using genome-wide association studies results on relative levels of T-cells in healthy individuals to measure the genetic contribution of T-cells in sarcoidosis entities. Results revealed that the genetic architecture of LS is highly influenced by genetic variants associated with CD8+ T-cells and CD4/CD8 ratio, explaining up to 7.94% and 6.49% of LS variation, respectively; whereas, the genetic architecture of non-LS is minimally influenced by T-cells, explaining a phenotypic variation of <1%. Moreover, pleiotropy assessment between T-cells and LS/non-LS associated-variants led to the discovery of highly scored pathway maps that shared common factors related to antigen presentation and T-cell regulatory mechanisms. Differences in significant polygenic scores, presence of pleiotropy, and distinct genetic factors provide further insights on how genetic variants and genes associated with relative levels of T-cell subtypes contribute differently to sarcoidosis phenotypes.