The polyamine-regulating enzyme SSAT1 impairs tissue regulatory T cell function in chronic cutaneous inflammation.

Regulatory T (T) cells are a critical immune component guarding against excessive inflammation. T cell dysfunction can lead to chronic inflammatory diseases with current therapies aimed at inhibiting effector T cells rather than rescuing T cell function. We utilized single-cell RNAsequencing data from patients with chronic inflammation to identify SAT1, the gene encoding spermidine/spermine N1-acetyltransferase (SSAT), as a driver of skin-resident T cell dysfunction. CRISPRa-driven SAT1 expression in human skin-derived T cells impaired their suppressive function and induced a pro-inflammatory phenotype. During cutaneous type-17 inflammation, keratinocyte 4-1BBL induces SAT1 on T cells. In a mouse model of psoriasis, pharmacological inhibition of SSAT rescued T cell number and function. Together, these data show that SAT1 expression has severe functional consequences on T cells and suggest a therapeutic target to treat chronic inflammatory disease.