Date published: 2025-9-20

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CD27L Inhibitors

CD27 Ligand (CD27L) Inhibitors are a group of chemical entities designed to modulate the activity of CD27 Ligand (CD27L), also known as CD70. CD27L is a critical component in the immune system, involved in the regulation of T-cell and B-cell responses. Its interaction with the CD27 receptor is essential for the activation and survival of lymphocytes. Direct chemical inhibition of CD27L is not well-established, but modulation of its expression or function can be achieved indirectly through the manipulation of immune signaling pathways and cellular processes. Compounds like Cyclosporin A, Rapamycin, and FK506 are immunosuppressants that act by inhibiting key signaling molecules within lymphocytes, such as calcineurin and mTOR. These inhibitors can indirectly affect the expression of CD27L by altering T-cell activation and function. For instance, the inhibition of calcineurin leads to reduced activation of the transcription factor NFAT, which is involved in the expression of various immune response genes, including CD27L. Glucocorticoids like Dexamethasone exert broad anti-inflammatory and immunosuppressive effects. Their action can lead to a downregulation of various immune-related genes, possibly impacting CD27L expression. Similarly, agents such as Methotrexate and Mycophenolate mofetil target cellular proliferation and metabolism in immune cells, influencing the regulation of CD27L. Other compounds, including JAK inhibitors (e.g., Tofacitinib) and proteasome inhibitors like Bortezomib, modulate signaling pathways and protein degradation processes, respectively, in immune cells. These actions can indirectly affect the dynamics of CD27L expression and function.

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