Date published: 2025-10-31

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IFN-α7 Activators

The activators of IFN-α7 operate through distinct molecular pathways to enhance its activity. Certain small molecules have been found to act on adenylyl cyclase to elevate intracellular cAMP levels, indirectly promoting IFN-α7 action via protein kinase A signaling. Others target the SIRT1 pathway, which modulates transcription factors to possibly enhance IFN-α7 expression. Some compounds exert their effects by inhibiting NF-κB, a transcription factor that generally suppresses interferon signaling pathways; the inhibition of NF-κB thereby relieves the suppression and may lead to increased IFN-α7 activity. Additionally, there are molecules that stabilize transcription factors such as p53, which are known to upregulate IFN-α7 through specific response elements, thereby promoting its expression and functional activity.

Moreover, specific activators work by inhibiting proteins like HMGB1, which are involved in suppressing the interferon response, thus potentially enhancing the activity of IFN-α7. Others stimulate peroxisome proliferator-activated receptor alpha, which may lead to transcriptional upregulation of IFN-α7. Some agents interfere with kinase activity, altering phosphorylation states and potentially favoring IFN-α7 signaling. There are also flavonoids that modulate phosphoinositide 3-kinases, which could result in enhanced signaling of IFN-α7. Furthermore, epigenetic modulation through inhibition of DNA methyltransferases can lead to changes in the methylation status of the IFN-α7 gene, potentially increasing its expression.

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