Biography
Leonardo M.R. Ferreira, Ph.D. is a molecular immunologist and human genome engineer in the laboratories of Dr. Qizhi Tang (Department of Surgery) and Dr. Jeffrey Bluestone (Diabetes Center) at UCSF.
Dr. Ferreira has a B.Sc. in biochemistry from the University of Coimbra, Portugal, and received a Ph.D. in biochemistry from Harvard University in 2016. During his doctoral studies, under the supervision of Dr. Jack Strominger and Dr. Chad Cowan at Harvard’s Department of Stem Cell and Regenerative Biology, he focused on studying immune tolerance using pregnancy as a model, as well as on developing new tools to edit the genome of primary human T cells.
Currently, Dr. Ferreira is working to develop the next generation of chimeric antigen receptors for regulatory T cell therapy, aiming to establish tolerance in the contexts of autoimmune disease and transplant rejection.
Videos
Education
Harvard University, Cambridge, Massachusetts, Ph.D., Biochemistry, 2016
Harvard University, Cambridge, Massachusetts, A.M., Biology, 2013
University of Coimbra, Coimbra, Portugal, B.Sc., Biochemistry, 2011
Tang Lab, Department of Surgery. 2016 -
Bluestone Lab, UCSF Diabetes Center, 2016 -
Ferreira LMR, Bluestone JA, Tang Q. Designing the next generation of chimeric antigen receptors for regulatory T cell therapy. Oral presentation, Federation of Clinical Immunology Societies (FOCIS), Chicago, Illinois, 2017, (Best Poster Award; FOCIS Travel Award)
Ferreira LMR, Meissner TB, Mikkelsen T, O'Donnell C, Sherwood R, Mallard W, Rinn J, Cowan, CA, Strominger JL. Long-range chromatin interactions control trophoblast-restricted HLA-G expression during pregnancy. Oral presentation, American Association of Immunologists (AAI), New Orleans, Louisiana, 2015 (AAI Travel Award)
In the News
Research Narrative
The adaptive immune system has evolved to specifically recognize and destroy a virtually infinite variety of pathogens, while remaining unresponsive towards self-tissues, a state known as immune tolerance. T cell-based antigen-specific immune tolerance was first postulated in 1970. Yet, it was not until the 1990s that the identity of the cell type responsible for this phenomenon was firmly established: regulatory T cells (Tregs).
Manipulating human Tregs offers the unprecedented opportunity to induce tolerance in a clinical setting, potentially providing cures for autoimmune disease and transplant rejection. However, vanishingly low numbers of antigen-specific Tregs and Treg instability upon prolonged expansion have hampered the implementation of Treg-based therapies.
Chimeric antigen receptor (CAR) technology has greatly expedited the generation of tumor antigen-specific effector T (Teff) cells. CARs are synthetic receptors comprising an extracellular antigen-binding domain and an intracellular signaling domain that allow for potent T cell activation directly downstream of antigen recognition.
Adoption of the CAR platform for Treg engineering represents a promising strategy to generate custom-made antigen-specific Tregs for therapy. Yet, there are marked differences in signaling and function between Tregs and Teff cells. My goal is to design the next generation of CARs for Treg therapy, aiming to establish tolerance in the contexts of autoimmune disease and transplant rejection.
Research Interests
Immune tolerance