Yannick Bulliard ¹ Robert Freeborn ¹ Molly Javier Uyeda ¹ Daryl Humes ¹ Ryan Bjordhal ¹ David de Vries ¹ Maria Grazia Roncarolo ^1,2*

• ¹ Tr1X, Inc., San Diego, United States
• ² Stanford University, Stanford, California, United States

Autoimmune diseases, characterized by the immune system's attack on the body's own tissues, affect 12 millions of people worldwide. Current treatments, which primarily rely on broad immunosuppression 13 and symptom management, are often associated with significant adverse effects and necessitate 14 lifelong therapy. This review explores the next generation of therapies for immune-mediated diseases, 15 including chimeric antigen receptor (CAR) T cell and regulatory T cell (Treg)-based approaches, which 16 offer the prospect of targeted, durable disease remission. Notably, we highlight the emergence of 17 CD19-targeted CAR T cell therapies, and their ability to drive sustained remission in B cell-mediated 18 autoimmune diseases, suggesting a possible paradigm shift. Further, we discuss the therapeutic 19 potential of Type 1 and FOXP3 + CAR Treg cells, which aim to achieve localized immune modulation 20 by targeting their activity to specific tissues or cell types, thereby minimizing the risk of generalized 21 immunosuppression. By examining the latest advances in this rapidly evolving field, we underscore 22 the potential of these innovative cell therapies to address the unmet need for long-term remission and 23 potential tolerance induction in individuals with autoimmune and immune-mediated diseases. 24