Biosketch
Zhijian ‘James’ Chen is an Investigator of Howard Hughes Medical Institute, and George L. MacGregor Distinguished Chair in Biomedical Science and Professor in the Department of Molecular Biology at the University of Texas Southwestern Medical Center at Dallas. Chen discovered the regulatory role of ubiquitination in protein kinase activation in the NF-?B and MAP kinase pathways. In addition, he discovered the Mitochondrial Antiviral Signaling (MAVS) protein that reveals a new role of mitochondria in immunity. More recently, Chen discovered cyclic GMP-AMP synthase (cGAS) as a cytosolic DNA sensor and a new cyclic di-nucleotide signaling pathway that mediate innate immune responses in animal cells. Chen was born in Anxi county, China, in 1966, and graduated from Fujian Normal University with a B.S. degree in biology. He received his Ph.D. degree in Biochemistry from University of Buffalo in 1991. After his postdoctoral training at the Salk Institute and working in the biotech industry, He joined the faculty at UT Southwestern in 1997. For his work, Chen has received numerous honors including the National Academy of Science Award in Molecular Biology (2012) and the Merck Award from the American Society of Biochemistry and Molecular Biology (ASBMB, 2015).
Research Interests
Zhijian 'James' Chen's laboratory is interested in the mechanisms of cell signaling, inflammation and innate immunity. Using classical biochemical fractionation and reconstitution, his lab has discovered several new mechanisms and signaling pathways that are important for animal cells to defend against microbial infections and other noxious insults. They found that the protein ubiquitin, which is best known for targeting protein degradation, plays an important role in activating protein kinases in inflammatory pathways through a proteolysis-independent mechanism. They discovered the mitochondrial protein MAVS and delineated its role and mechanism in immune defense against RNA virus infections. More recently, the Chen lab discovered the enzyme cyclic GMP-AMP synthase (cGAS) and showed that it is the cytosolic DNA sensor that activates the host immune system by producing a novel second messenger, cyclic GMP-AMP (cGAMP). They are further dissecting the MAVS and cGAS-cGAMP pathways with the goal of developing new agents for the treatment or prevention of infectious diseases, autoimmune diseases and cancer.
Membership Type
Member
Election Year
2014
Primary Section
Section 43: Immunology and Inflammation
Secondary Section
Section 21: Biochemistry