Identification of TAPBPL as a novel negative regulator of T-cell function.
Yujun LinCheng CuiMin SuLawrence K SilbartHaiyan LiuJin ZhaoLang HeYuanmao HuangDexin XuXiaodan WeiQian DuLaijun LaiPublished in: EMBO molecular medicine (2021)
T cell stimulatory and inhibitory molecules are critical for the regulation of immune responses. In this study, we identify a novel T cell co-inhibitory molecule TAPBPL, whose amino acid sequence shares homology with known B7 family members. TAPBPL protein is expressed on resting and activated T cells, B cells, monocytes, and dendritic cells (DCs), as well as on some tumor tissues. The putative TAPBPL receptor is expressed on activated CD4 and CD8 T cells. A soluble recombinant human TAPBPL-IgG Fc (hTAPBPL-Ig) fusion protein inhibits the proliferation, activation, and cytokine production of both mouse and human T cells in vitro. In vivo administration of hTAPBPL-Ig protein attenuates experimental autoimmune encephalomyelitis (EAE) in mice. Furthermore, an anti-TAPBPL monoclonal antibody neutralizes the inhibitory activity of hTAPBPL-Ig on T cells, enhances antitumor immunity, and inhibits tumor growth in animal models. Our results suggest that therapeutic intervention of the TAPBPL inhibitory pathway may represent a new strategy to modulate T cell-mediated immunity for the treatment of cancer, infections, autoimmune diseases, and transplant rejection.
Keyphrases
- amino acid
- dendritic cells
- monoclonal antibody
- immune response
- recombinant human
- randomized controlled trial
- binding protein
- protein protein
- regulatory t cells
- gene expression
- transcription factor
- signaling pathway
- heart rate
- heart rate variability
- squamous cell
- induced pluripotent stem cells
- toll like receptor
- high fat diet induced
- metabolic syndrome
- young adults
- childhood cancer
- combination therapy
- insulin resistance
- skeletal muscle
- lymph node metastasis
- adipose tissue
- peripheral blood
- pluripotent stem cells
- inflammatory response