Date published: 2025-9-15

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PRAMEF11 Activators

PRAMEF11, a member of the PRAME (Preferentially Expressed Antigen in Melanoma) family, is a gene that has garnered interest due to its expression profile in various tissues. The PRAME family of genes is known for their role in normal cellular functions and their atypical expression in certain types of cells under specific conditions. PRAMEF11's function in normal physiology remains an area of ongoing research, yet it is understood that the gene may play a role in the intricate ballet of gene expression regulation. The expression of PRAMEF11, like many genes, is controlled by a network of epigenetic and transcriptional mechanisms that ensure the proper level of expression in response to a variety of cellular signals and environmental factors.

The potential inducers of PRAMEF11 expression encompass a diverse array of chemical compounds that can instigate a complex cascade of intracellular events, culminating in the upregulation of this gene. Compounds such as 5-Azacytidine and Trichostatin A, known for their ability to modify epigenetic marks, could remove repressive methylation patterns or increase acetylation at the PRAMEF11 locus, clearing the way for transcriptional machinery. Similarly, molecules that interact with intracellular receptor pathways, such as retinoic acid or synthetic estrogens like diethylstilbestrol, might bind to their cognate receptors and promote transcription factor recruitment to the PRAMEF11 promoter. Other compounds, including those like sulforaphane and curcumin, might upregulate PRAMEF11 indirectly by activating broader stress response pathways or modifying the activity of transcription factors that, in turn, target the PRAMEF11 gene. The exact molecular interplay between these compounds and PRAMEF11 expression is a fascinating topic for research, offering a window into the dynamic nature of gene regulation.

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