Date published: 2025-11-2

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CIR Activators

CIR activators include a class of compounds that can modulate epigenetic markers and influence signaling pathways indirectly associated with the transcriptional repression activities of CIR. These activators typically function by altering the acetylation and methylation status of histones, thereby affecting the chromatin state and the transcriptional dynamics of the genes involved in Notch signaling, where CIR acts as a corepressor.

Chemical activators such as HDAC inhibitors, like Valproic Acid, Trichostatin A, and SAHA, can lead to increased histone acetylation, which may reduce the binding affinity of CIR to the chromatin, thus relieating its repressive effects on gene transcription. This modification in the chromatin landscape can facilitate a more transcriptionally permissive environment. Similarly, DNA methyltransferase inhibitors, like 5-Azacytidine, could disrupt CIR's ability to maintain a repressed chromatin state by causing DNA demethylation, thereby enhancing the expression of target genes. On the other hand, small molecules like DAPT, by modulating the cleavage of Notch receptors, may alter the Notch signaling pathway's flux and consequently its interaction with CIR. Compounds like Lithium Chloride can indirectly influence CIR activity by inhibiting GSK-3, increasing beta-catenin levels and affecting the gene regulatory networks associated with Notch signaling.

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