Chemical inhibitors of B7h can exert their inhibitory action through various cellular pathways that are crucial for the regulation and expression of this protein. Cyclosporin A and Ascomycin, both immunosuppressive agents, can inhibit calcineurin, which is vital for the activation of T-cells, leading to the suppression of B7h expression on antigen-presenting cells. By impeding T-cell activation, these chemicals ensure that the upregulation of B7h, which could otherwise be stimulated during immune responses, is kept in check. Similarly, Rapamycin binds to FKBP-12 and inhibits the mTOR pathway, which is instrumental in T-cell proliferation and can also govern the levels of B7h expression. The interruption of mTOR signaling can thus result in decreased B7h expression on cells that interact with T-cells.
Furthermore, inhibitors like WZ4002, PD98059, SB203580, and SP600125 target different kinases involved in T-cell activation. WZ4002, a selective EGFR inhibitor, hinders T-cell proliferation, which can otherwise increase B7h expression. PD98059 targets MEK in the MAPK/ERK pathway, and SB203580 targets p38 MAPK, both of which are important for T-cell activation that could induce B7h expression. SP600125, a JNK inhibitor, operates within the same framework, ensuring that T-cell activation does not result in heightened B7h expression. LY294002 and Wortmannin are PI3K inhibitors that prevent the activation of T-cells, leading to reduced B7h expression. Trichostatin A, an HDAC inhibitor, alters chromatin structure and gene expression, which can result in the suppression of genes involved in the immune response, including B7h. BAY 11-7082 inhibits NF-κB, a transcription factor that modulates immune cell activation, thereby potentially reducing B7h expression. Lastly, Sotrastaurin, a Protein kinase C inhibitor, suppresses T-cell activation, which is essential for maintaining B7h expression on antigen-presenting cells. By disrupting these specific signaling pathways, each chemical contributes to the functional inhibition of B7h by ensuring that its expression is not upregulated in the context of immune cell activation.
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