Date published: 2025-11-7

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ZFP14 Activators

ZFP14 can influence the protein's activity in various ways, primarily through the modulation of its DNA-binding ability and the alteration of the chromatin landscape in which it operates. For example, zinc pyrithione can enhance ZFP14's DNA-binding affinity by binding to its zinc finger domain, which is crucial for its ability to interact with DNA. This results in a more stabilized protein conformation and effectively increases ZFP14's activity. Similarly, disulfiram and pyrrolidine dithiocarbamate can chelate zinc ions, potentially increasing the local concentration of zinc available for ZFP14, thus facilitating its proper function. On the other hand, Trichostatin A and SAHA (Vorinostat) are inhibitors of histone deacetylases. Their action leads to a relaxed chromatin structure, granting ZFP14 greater access to DNA, and consequently, higher transcriptional activity.

Other activators work by influencing the cellular conditions to favor ZFP14's function. Resveratrol activates sirtuins, which can lead to deacetylation of histones, thus potentially enabling ZFP14 to bind to DNA more effectively. Spermidine can trigger autophagy, which might degrade proteins that otherwise inhibit ZFP14, freeing it to activate its target genes. Similarly, 5-Aza-2'-deoxycytidine's inhibition of DNA methyltransferases results in DNA hypomethylation, which can also enhance the DNA binding of ZFP14, leading to its activation. Ascorbic acid maintains ZFP14's function by reducing oxidative damage. Genistein and Epigallocatechin gallate influence phosphorylation patterns and DNA methylation respectively, each leading to conditions that may enhance the DNA-binding activity of ZFP14. Lastly, sodium butyrate's inhibition of histone deacetylase creates a chromatin environment conducive to ZFP14 binding to DNA, thus facilitating its activation. Each of these chemicals contributes to the activation of ZFP14 through distinct mechanisms that ensure the protein's effective engagement with its DNA targets.

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