The female-biased factor VGLL3 drives cutaneous and systemic autoimmunity
Male
0303 health sciences
Autoimmunity
Mice, Transgenic
3. Good health
Disease Models, Animal
Mice
03 medical and health sciences
Sex Factors
Gene Expression Regulation
Lupus Erythematosus, Cutaneous
Animals
Humans
Lupus Erythematosus, Systemic
Female
Skin
Transcription Factors
DOI:
10.1172/jci.insight.127291
Publication Date:
2019-04-17T15:09:08Z
AUTHORS (27)
ABSTRACT
Autoimmune disease is 4 times more common in women than men. This bias is largely unexplained. Female skin is "autoimmunity prone," showing upregulation of many proinflammatory genes, even in healthy women. We previously identified VGLL3 as a putative transcription cofactor enriched in female skin. Here, we demonstrate that skin-directed overexpression of murine VGLL3 causes a severe lupus-like rash and systemic autoimmune disease that involves B cell expansion, autoantibody production, immune complex deposition, and end-organ damage. Excess epidermal VGLL3 drives a proinflammatory gene expression program that overlaps with both female skin and cutaneous lupus. This includes increased B cell-activating factor (BAFF), the only current biologic target in systemic lupus erythematosus (SLE); IFN-κ, a key inflammatory mediator in cutaneous lupus; and CXCL13, a biomarker of early-onset SLE and renal involvement. Our results demonstrate that skin-targeted overexpression of the female-biased factor VGLL3 is sufficient to drive cutaneous and systemic autoimmune disease that is strikingly similar to SLE. This work strongly implicates VGLL3 as a pivotal orchestrator of sex-biased autoimmunity.
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