Date published: 2025-9-17

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ZFP772 Inhibitors

Chemical inhibitors of zinc finger protein 772 can exert their inhibitory effects through various molecular pathways that are essential for the protein's function. Triptolide targets the NF-κB pathway, which zinc finger protein 772 utilizes for DNA binding and regulation of transcription. By inhibiting this pathway, triptolide effectively reduces the DNA binding activity of the protein, leading to a functional inhibition. Similarly, PD98059 disrupts the MEK/ERK pathway which is crucial for the signal transduction processes involving zinc finger protein 772. This results in a lack of necessary phosphorylation signals, crucial for the protein's activity. SB203580 and SP600125 are other examples, targeting the p38 MAP Kinase and JNK respectively. The inhibition of these kinases by SB203580 and SP600125 can lead to a decrease in the functional activity of zinc finger protein 772 by altering its signal transduction and post-translational modification status.

Furthermore, the PI3K/Akt pathway, pivotal for the full activation and stability of zinc finger protein 772, can be inhibited by chemicals like LY294002 and Wortmannin, which act as PI3K inhibitors. This directly results in a reduction of zinc finger protein 772's activity. Rapamycin and U0126 add to this arsenal by inhibiting mTOR and MEK1/2, leading to a decrease in cellular growth signals and activation of transcription factors that zinc finger protein 772 modulates. IKK-16's inhibition of the IKK complex reduces NF-κB nuclear translocation, which is likely to regulate zinc finger protein 772 activity. Proteasome inhibitors such as MG132 and Bortezomib result in an accumulation of regulatory proteins that can inhibit the DNA binding activity of zinc finger protein 772, preventing its interaction with target DNA sequences. Lastly, Thapsigargin disrupts calcium homeostasis by inhibiting SERCA, an essential process for the function of many zinc finger proteins, including zinc finger protein 772, culminating in the inhibition of its activity. Through these diverse yet specific pathways, each chemical collectively contributes to the functional inhibition of zinc finger protein 772.

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