Date published: 2025-10-11

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ZNF429 Inhibitors

Chemical inhibitors of ZNF429 utilize a range of mechanisms to disrupt its function within cellular signaling pathways. Staurosporine serves as a potent kinase inhibitor, directly inhibiting the phosphorylation of ZNF429, which is crucial for its activation and function. Similarly, rapamycin targets mTOR, a kinase that may play a role in ZNF429's phosphorylation state. By inhibiting mTOR, rapamycin can suppress the activation of ZNF429, thereby inhibiting its function. LY294002 and Wortmannin both target PI3K, which is upstream in the signaling pathway and can reduce the phosphorylation of proteins that regulate the activity of ZNF429, leading to an overall decrease in its functional activity. U0126 and PD98059, as MEK inhibitors, disrupt the MAPK/ERK pathway, which is involved in the regulation of various proteins that could be essential for ZNF429's functionality. By preventing this pathway from functioning normally, these inhibitors can suppress ZNF429 activity.

In addition to these, SP600125 inhibits JNK, another kinase that can be involved in phosphorylating proteins that interact with ZNF429. This inhibition can lead to a decrease in ZNF429's functional activity. SB203580 specifically inhibits p38 MAPK, which also could play a role in the regulation of ZNF429, leading to its functional inhibition. Dasatinib, by inhibiting Src family kinases, prevents the phosphorylation of proteins that are necessary for the functional activity of ZNF429. H-89 targets PKA, thereby potentially leading to a reduction in the phosphorylation of proteins that regulate ZNF429 activity. Chelerythrine inhibits PKC, which is implicated in the phosphorylation of proteins interacting with ZNF429, thus inhibiting its activity. Lastly, Bortezomib inhibits the proteasome, which can lead to an increase in proteins that negatively regulate ZNF429, resulting in its inhibition.

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