Rare genetic variants provide a mechanistic basis for immune imbalance in IgG4-related disease
Dominic J. Ciavatta
Dominic J. Ciavatta
Published August 15, 2024
Citation Information: J Clin Invest. 2024;134(16):e183396. https://doi.org/10.1172/JCI183396.
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Commentary

Rare genetic variants provide a mechanistic basis for immune imbalance in IgG4-related disease

Abstract

Autoimmune diseases are commonly associated with a polygenic inheritance pattern. In rare instances, causal monogenic variants have been identified. The study by Liu et al. in this issue of the JCI provides an example of monogenic variants occurring in patients with IgG4-related disease (IgG4-RD). The authors investigated a familial cluster of IgG4-RD that consisted of an affected father and two daughters; the mother was unaffected. Genome sequencing of this quad identified a variant in IKZF1 (encoding IKAROS) and another variant in UBR4 (encoding E3 ubiquitin ligase). Both variants were present in the father and both daughters but absent in the unaffected mother. Using multidimensional profiling of immune cells and functional experiments in primary cells, the authors determined a molecular pathway contributing to T cell activation in IgG4-RD. Importantly, the characterization of these variants provides insights into pathogenic mechanisms in IgG4-RD and, potentially, other autoimmune diseases.

Authors

Dominic J. Ciavatta

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Figure 1

Patients with IgG4-RD possess genetic variants responsible for Th2 polarization and T cell activation.

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Patients with IgG4-RD possess genetic variants responsible for Th2 polar...
(A) Three members of a family were affected by IgG4-RD: the father (teal square) and two daughters (teal circles). The mother was unaffected (white circle). (B) Rare variants were detected in the genome sequence of the affected individuals. The GOF IKAROS-R183H variant increases FYN expression, and the LOF UBR4-C4179Ter variant inhibits clearance of the tyrosine phosphatase CD45, which removes inhibitory phosphate, sparing phosphorylation at the activating tyrosine residue and leading to activation of FYN. The consequence of these variants for FYN stabilizes JunB to drive Th2 response genes and T cell activation.