Date published: 2025-9-11

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BRMS1L Activators

BRMS1L is a transcriptional repressor that plays a role in gene regulation, and its activity can be modulated by various chemical compounds through distinct pathways. Compounds that increase intracellular cAMP levels, such as adenylyl cyclase activators, can enhance the activity of transcription factors that govern the transcription of genes regulated by BRMS1L. Similarly, cAMP analogs that activate protein kinase A result in the phosphorylation of specific proteins that interact with BRMS1L, potentially augmenting its transcriptional repression capabilities. This is further supported by compounds that modify chromatin structure through the inhibition of histone deacetylases, which facilitate the access of transcription factors to DNA, consequently increasing the transcription of genes under BRMS1L control and enhancing its function. Furthermore, DNA methyltransferase inhibitors contribute to the activation of BRMS1L by promoting the hypomethylation of its target genes, which is known to correlate with increased transcription.

In addition to epigenetic modulators, other molecules contribute to the functional activation of BRMS1L by influencing the transcriptional machinery. Sirtuin activators, for instance, deacetylate proteins including transcription factors, potentially boosting BRMS1L's ability to repress its target genes. Histone deacetylase inhibitors, such as sodium butyrate, can lead to hyperacetylation of histones, which promotes the transcription of BRMS1L-regulated genes, implying an enhancement of its repressive function. The activation of nuclear receptors by compounds like retinoic acid alters gene expression patterns, some of which are governed by BRMS1L, thereby modulating its activity. Additional mechanisms include inhibition of histone methyltransferases and bromodomain-containing proteins, which can affect histone methylation and acetylation states, respectively.

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