4.7 Article

GWAS and autoimmunity: What have we learned and what next

Journal

JOURNAL OF AUTOIMMUNITY
Volume 133, Issue -, Pages -

Publisher

ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD
DOI: 10.1016/j.jaut.2022.102922

Keywords

Autoimmunity; Liver; GWAS; Genetic variants; Fine mapping; eQTL

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Autoimmune diseases are common and complex, with a polygenic nature. Recent advances in genomics have improved the understanding of the effects of genetic variants on target tissues and immune cells. However, there are still gaps in research and future directions to explore.
Autoimmune diseases are common conditions characterized by loss of tolerance, female predominance and a remarkable heterogeneity among different populations. Most often they are polygenic and several genetic loci have been linked with the risk of developing autoimmune diseases. However, causal inference is difficult. When the genomic revolution began there were high hopes of translating fast genetic analyses to the bedside but this has proven to be challenging. Nonetheless, over the last decade, fine-mapping strategies have greatly improved; one of the most significant research lines focuses on the in vivo and ex vivo definition of the effect of genetic variants within the target tissues and within specific subpopulations of immune cells that are involved in the disease pathogenesis. This strategy also includes the longitudinal tracking of a large number of immunophe-notypes in many individuals to build a large reference atlas for variant characterization. In this review, we discuss the results obtained by GWAS in autoimmune diseases and review recent advances in fine mapping strategies. More importantly, we discuss gaps and future directions.

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