Date published: 2025-9-17

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ILT-8 Activators

ILT-8 activators comprise a diverse array of chemical compounds that enhance the functional activity of ILT-8 through distinct but interconnected signaling pathways. Forskolin, through its activation of adenylate cyclase leading to increased cAMP, activates PKA, which is known to phosphorylate proteins and influence immune response mechanisms, thereby potentiating ILT-8 signaling indirectly. Similarly, resveratrol's activation of SIRT1 and the subsequent modulation of NF-kB acetylation foster an environment conducive to the enhanced activity of ILT-8 by fine-tuning immune regulatory processes. Curcumin further contributes to this enhancement by inhibiting NF-kB and STAT3, pivotal in the regulation of inflammation and immune response, creating a pathway bias that favors ILT-8 activity. The inhibition of kinases by EGCG shifts cellular signaling in favor of pathways associated with ILT-8, indirectly increasing its activity.

Furthermore, capsaicin's stimulation of the TRPV1 receptor induces calcium influx, activating calcium-dependent signaling pathways that can augment the function of ILT-8 in immune responses. Quercetin's modulation of PI3K and PKC signaling cascades indirectly supports ILT-8 activity by influencing immune function pathways. Sulforaphane, through Nrf2 activation, orchestrates an antioxidant response that can skew signaling pathways towards those involving ILT-8 function in immunity. Lithium chloride, by inhibiting GSK-3 enzymes, and sodium butyrate and nicotinamide, both acting as HDAC inhibitors, alter gene expression and inflammation pathways, culminating in an elevated ILT-8 activity. Omega-3 fatty acids alter inflammatory signaling, inherently enhancing ILT-8's role within these processes, while caffeine's inhibition of phosphodiesterases leads to increased cAMP and subsequent PKA activation, further promoting ILT-8's involvement in modulating immune responses.

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