AI Article Synopsis

  • Biologics targeting TNF family receptors can be effective for treating immune diseases, with antibodies to 4-1BB (CD137) currently undergoing clinical trials for both cancer and autoimmune conditions.
  • Recent research indicates that the action of agonist anti-4-1BB, which helps reduce autoimmune and allergic inflammation, relies heavily on Galectin-9 (Gal-9), a protein that binds directly to 4-1BB.
  • Gal-9 enhances 4-1BB’s function by promoting its aggregation and signaling in various immune cells, and its interaction is also conserved in humans, suggesting potential for targeted clinical therapies involving 4-1BB and similar proteins.

Article Abstract

Biologics to TNF family receptors are prime candidates for therapy of immune disease. Whereas recent studies have highlighted a requirement for Fcγ receptors in enabling the activity of CD40, TRAILR, and GITR when engaged by antibodies, other TNFR molecules may be controlled by additional mechanisms. Antibodies to 4-1BB (CD137) are currently in clinical trials and can both augment immunity in cancer and promote regulatory T cells that inhibit autoimmune disease. We found that the action of agonist anti-4-1BB in suppressing autoimmune and allergic inflammation was completely dependent on Galectin-9 (Gal-9). Gal-9 directly bound to 4-1BB, in a site distinct from the binding site of antibodies and the natural ligand of 4-1BB, and Gal-9 facilitated 4-1BB aggregation, signaling, and functional activity in T cells, dendritic cells, and natural killer cells. Conservation of the Gal-9 interaction in humans has important implications for effective clinical targeting of 4-1BB and possibly other TNFR superfamily molecules.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4076583PMC
http://dx.doi.org/10.1084/jem.20132687DOI Listing

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