Date published: 2025-12-28

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ZNF134 Inhibitors

Chemical inhibitors of ZNF134 target various cellular pathways to exert their inhibitory effects on the protein's function. Alsterpaullone and Indirubin-3'-monoxime disrupt the normal cell cycle by inhibiting cyclin-dependent kinases and GSK-3β, respectively. This inhibition can arrest the cell cycle, thereby preventing ZNF134 from carrying out its regulatory roles during specific cell cycle phases. Similarly, the JNK inhibitor SP600125 can alter transcription factor activities which are critical for ZNF134's regulatory functions. In addition to these, Y-27632 targets ROCK kinases, whose role in cytoskeletal organization is critical for the proper intracellular localization and consequent function of ZNF134. By disrupting these kinases, Y-27632 can impede the correct positioning and functioning of ZNF134 within the cell.

Moreover, inhibitors such as SB203580, PD98059, and U0126 interfere with the MAPK/ERK pathway, a key signaling route involved in the regulation of protein functions. By preventing the necessary phosphorylation events within this pathway, these inhibitors can suppress the activity of ZNF134. LY294002, as a PI3K inhibitor, and rapamycin, as an mTOR inhibitor, act similarly by hindering pathways that control protein phosphorylation and cell growth, respectively, ultimately decreasing ZNF134's activity. Disruption of calcium homeostasis through the use of Thapsigargin, which inhibits the SERCA pump, can also affect ZNF134 by impacting its folding or stability. Brefeldin A interrupts intracellular protein transport by inhibiting ADP-ribosylation factor, which could result in the mislocalization of ZNF134, hindering its function. Finally, Cyclopamine directly inhibits the Hedgehog signaling pathway, which can suppress the gene regulation functions of ZNF134 by blocking this critical developmental signaling route. Each chemical's mode of action culminates in the functional inhibition of ZNF134, thereby dampening the protein's regulatory capacity within various biological contexts.

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