Date published: 2025-9-22

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RFX1 Inhibitors

RFX1 inhibitors as a chemical class encompass a range of compounds that indirectly affect the regulatory functions of RFX1, a DNA-binding protein implicated in the transcriptional control of several genes. These compounds achieve this by targeting associated signaling pathways and cellular processes that are prerequisite for RFX1's transcriptional activity. This includes modulation of chromatin structure, DNA methylation patterns, proteasome function, and various signaling cascades such as those mediated by AP-1 or NF-κB. For instance, compounds like JQ1 and I-BET151 disrupt the reading of acetylated histones by BET bromodomains, which is critical for the proper positioning of transcription factors such as RFX1 at gene promoters. SR11302 impedes AP-1, which may have downstream effects on the transcriptional programs involving RFX1.

Furthermore, the cellular transcriptional machinery can be affected by Triptolide, which targets the RNA polymerase II complex, a key player in the transcription of RFX1 target genes. Epigenetic modifiers like Decitabine and 5-Azacytidine alter DNA methylation status, which could change the genomic landscape that RFX1 interacts with, while MG132 disrupts proteasomal degradation, potentially leading to an accumulation of regulatory proteins that compete or interact with RFX1. Withaferin A and Curcumin alter the activity of NF-κB, a factor that can function cooperatively or antagonistically with RFX1. Agents like Chetomin and Epigallocatechin Gallate can interfere with protein-protein interactions and DNA methyltransferases respectively, thereby modulating the transcriptional activity where RFX1 plays a role. Finally, Oligomycin A's impact on cellular energy may indirectly affect RFX1's functionality due to the energy-dependent nature of transcriptional processes. These chemicals, through their varied modes of action, establish a broad and indirect approach to modulating RFX1 activity within the cell.

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