Date published: 2025-9-17

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ZFP414 Inhibitors

Chemical inhibitors of ZFP414 can influence its activity through various biochemical pathways, ensuring that this zinc finger protein's function is impeded. PD173074 acts by targeting the fibroblast growth factor receptors which are integral for certain signaling pathways that ZFP414 might be a part of; thus, it impedes its function indirectly. Similarly, LY294002 disrupts the PI3K/Akt pathway, a crucial signaling route for cell survival and proliferation, which can lead to a decrease in the activity of proteins like ZFP414 that may be regulated by this pathway. U0126 and PD98059 both target MEK1/2, with U0126 being selective and PD98059 more general, inhibiting the MAPK/ERK pathway and thereby reducing the phosphorylation and, consequently, the activity of downstream proteins, including ZFP414. Furthermore, SB203580 and SP600125 inhibit the p38 MAP kinase and c-Jun N-terminal kinase, respectively. The p38 MAP kinase plays a role in stress responses, and its inhibition can lead to altered function of proteins associated with this pathway, including ZFP414. The JNK pathway influences the phosphorylation of a wide array of proteins; SP600125's action can prevent this phosphorylation, thereby inhibiting ZFP414's function. Rapamycin targets mTOR, which is a central regulator of cell growth, and its inhibition could decrease the activity of ZFP414 if it is regulated by mTOR signaling. PP2 disrupts Src family kinase signaling, potentially affecting ZFP414 if it is part of this signaling network. Y-27632, as a ROCK inhibitor, can prevent the phosphorylation of Rho-associated kinase substrates, which could implicate ZFP414 if it is involved in Rho/ROCK signaling. Wortmannin, another PI3K inhibitor like LY294002, similarly can lead to a decrease in the activity of proteins in the PI3K/Akt pathway, potentially leading to the inhibition of ZFP414. Lastly, Alsterpaullone and Triptolide target the cyclin-dependent kinases and NF-κB, respectively. Alsterpaullone inhibits cell cycle progression, which can influence ZFP414 if it is linked to cell cycle regulation. Triptolide's inhibition of NF-κB suggests a decrease in the function of proteins regulated by this transcription factor, which could include ZFP414, resulting in its functional inhibition.

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