We report that the paracaspase Malt1 is required for the development and function of Treg cells. By generating Malt1 conditional knockout and protease dead mutant mice, we found Malt1-loss in Treg cells would lead to early-onset lethal autoimmune disease and the mice would die within 40 days after birth. Interestingly, mice with Treg specific inhibition of Malt1 protease activity develop spontaneous inflammatory disorders. SOURCE: Liqing ChengLinxin lab Tsinghua university

Pluto Bioinformatics

GSE124089: Malt1 protease is critical in maintaining function of Treg cells and may be a therapeutic target for anti-tumor immunity