# Mechanisms of genetic variants in TH2 autoimmunity

> **NIH NIH R01** · MAYO CLINIC ROCHESTER · 2024 · $606,229

## Abstract

PROJECT SUMMARY
Monogenic autoimmune diseases, while rare, offer a unique opportunity to develop models that enable a more
mechanistic understanding of the disease process, in particular, if the mutation is in the coding region and the
penetrance is high. We have identified a family, in which father and two daughters have Immunoglobulin G4-
related disease (IgG4-RD) while the mother is healthy. Exome sequencing identified shared mutations in the E3
ubiquitin ligase UBR4 (Cys4179Ter) and the transcription factor IKZF1 (IKAROS, Arg183His) genes in affected
family members. IgG4-RD is a systemic autoimmune disease manifesting as a fibrosing inflammation of major
salivary glands, orbits, pancreas, and retroperitoneal soft tissue, frequently associated with elevated serum IgG4
and IgE, increased peripheral eosinophilia and high rates of atopy/allergies. The pathogenesis of the disease is
essentially unknown. IKZF1 is a gene that has been associated with a variety of autoimmune manifestations,
without that pathogenetic pathways have been identified. Specifically, loss of function mutations cause immune
deficiencies combined with tissue inflammation, while IKZF1 haplotypes have been associated with SLE and
other autoimmune diseases in GWAS studies. The IKZF1 mutation identified here is unique in that it is a gain-
of-function (GOF) due to increasing DNA binding affinity. We propose that an understanding of the effect of the
GOF effects and their interaction with the proteome changes due UBR4 haploinsufficiency provides an
opportunity to define mechanisms that lead to defective tolerance and excessive TH2 polarization. We propose
a two-pronged approach. In Aims 1 and 2, we will build on our preliminary data that UBR4 haploinsufficiency
increases CD45 expression while GOF IKAROS increases FYN transcription. Aim 1 will determine whether
UBR4 and IKFZ1 GOF gene variants increase TCR signaling and break tolerance by upregulating CD45 and
FYN. Aim 2 will examine the model that FYN drives TH2 polarization by phosphorylating ITCH2 and preventing
the degradation of JunB. In these aims, we use a combination of human in vitro and mouse in vivo studies.
Therapeutic implications will be examined in models of allergic airway inflammation by pharmacological depletion
of IKAROS, as recently done for human SLE. In addition to these hypothesis-driven studies based on a large
body of preliminary data, we propose to continue an unbiased screening of the proteomic and transcriptomic
changes due to the gene variants to identify molecules that can be built into the current model. Aim 3 will
determine whether the biomarkers developed from studying this digenic disease have broader implications for
non-familial IgG4-RD disease as well as for other diseases that are characterized by an unopposed TH2
immunity.

## Key facts

- **NIH application ID:** 10934658
- **Project number:** 1R01AI184360-01
- **Recipient organization:** MAYO CLINIC ROCHESTER
- **Principal Investigator:** JORG J GORONZY
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $606,229
- **Award type:** 1
- **Project period:** 2024-07-05 → 2029-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10934658

## Citation

> US National Institutes of Health, RePORTER application 10934658, Mechanisms of genetic variants in TH2 autoimmunity (1R01AI184360-01). Retrieved via AI Analytics 2026-05-26 from https://api.ai-analytics.org/grant/nih/10934658. Licensed CC0.

---

*[NIH grants dataset](/datasets/nih-grants) · CC0 1.0*