RT Journal Article ID 401710425da8e08e A1 Strle, Klemen A1 Zhou, Jian-Hua A1 Shen, Wen-Hong A1 Broussard, Suzanne R. A1 Johnson, Rodney W. A1 Freund, Gregory G. A1 Dantzer, Robert A1 Kelley, Keith W. T1 lnterleukin-10 in the Brain JF Critical Reviews™ in Immunology JO CRI YR 2001 FD 2001-10-01 VO 21 IS 5 OP 23 AB Interleukin (IL)-10 is synthesized in the central nervous system (CNS) and acts to limit clinical symptoms of stroke, multiple sclerosis, Alzheimer's disease, meningitis, and the behavioral changes that occur during bacterial infections. Expression of IL-10 is elevated during the course of most major diseases in the CNS and promotes survival of neurons and all glial cells in the brain by blocking the effects of proapoptotic cytokines and by promoting expression of cell survival signals. Stimulation of IL-10 receptors regulates numerous life- or death-signaling pathways—including Jakl/Stat3, PI 3-kinase, МАРК, SOCS, and NF-kВ—ultimately promoting cell survival by inhibiting both ligand- and mitochondrial-induced apoptotic pathways. IL-10 also limits inflammation in the brain; it does so by three major pathways: (1) reducing synthesis ofproinflammatory cytokines, (2) suppressing cytokine receptor expression, and (3) inhibiting receptor activation. Finally, IL-10 induces anergy in brain-infiltrating Т cells by inhibiting cell signaling through the costimulatory CD28-CD80/86 pathway. The multiple functions of IL-10 in the brain will create new and intriguing vistas that will promote a better understanding of neurodegenerative diseases. These discoveries could lead to development of innovative approaches for the use of anti-inflammatory cytokines in major debilitating diseases of the CNS. PB Begell House LK https://www.dl.begellhouse.com/journals/2ff21abf44b19838,5ce6ad235835b45a,401710425da8e08e.html