4.8 Article

Diagnostic and therapeutic potential of RNASET2 in Crohn's disease: Disease-risk polymorphism modulates allelic-imbalance in expression and circulating protein levels and recombinant-RNASET2 attenuates pro-inflammatory cytokine secretion

Journal

FRONTIERS IN IMMUNOLOGY
Volume 13, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fimmu.2022.999155

Keywords

Crohn's disease; allelic imbalance; inflammation; human; gene regulation; cytokine

Categories

Funding

  1. F. Widjaja Foundation
  2. National Institute of Diabetes Digestive & Kidney Diseases
  3. [RO1 DK117893]

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RNASET2 gene variants are associated with risk for autoimmune diseases like Crohn's disease. There is a relationship between RNASET2, T cell activation, mucosal inflammation, and disease severity. The variants are associated with decreased mRNA expression and clinical characteristics of severe Crohn's disease. The study found that the variants affect transcriptional and post-transcriptional mechanisms, and overexpression or treatment with RNASET2 can reduce IFN-gamma secretion. Preoperative RNASET2 protein levels are decreased in severe Crohn's disease patients and increase post-operatively after removal of the inflamed region.
Ribonuclease T2 gene (RNASET2) variants are associated in genome wide association studies (GWAS) with risk for several autoimmune diseases, including Crohn's disease (CD). In T cells, a functional and biological relationship exists between TNFSF15-mediated enhancement of IFN-gamma production, mucosal inflammation and RNASET2. Disease risk variants are associated with decreased mRNA expression and clinical characteristics of severe CD; however, functional classifications of variants and underlying molecular mechanisms contributing to pathogenesis remain largely unknown. In this study we demonstrate that allelic imbalance of RNASET2 disease risk variant rs2149092 is associated with transcriptional and post-transcriptional mechanisms regulating transcription factor binding, promoter-transactivation and allele-specific expression. RNASET2 mRNA expression decreases in response to multiple modes of T cell activation and recovers following elimination of activator. In CD patients with severe disease necessitating surgical intervention, preoperative circulating RNASET2 protein levels were decreased compared to non-IBD subjects and rebounded post-operatively following removal of the inflamed region, with levels associated with allelic carriage. Furthermore, overexpression or treatment with recombinant RNASET2 significantly reduced IFN-gamma secretion. These findings reveal that RNASET2 cis- and trans-acting variation contributed regulatory complexity and determined expression and provide a basis for linking genetic variation with CD pathobiology. These data may ultimately identify RNASET2 as an effective therapeutic target in a subset of CD patients with severe disease.

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