Date published: 2025-9-15

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C2orf57 Activators

Retinoic Acid engages nuclear receptors to regulate gene expression, which includes proteins involved in transcription and DNA repair processes. By inhibiting DNA methyltransferases, 5-Azacytidine alters the methylation landscape of the genome, leading to the activation of genes that could express proteins like C2orf57. Similarly, histone deacetylase inhibitors such as Trichostatin A, Sodium Butyrate, and Suberoylanilide Hydroxamic Acid alter chromatin architecture, enhancing the transcriptional activity of genes by increasing histone acetylation and promoting a transcriptionally active chromatin state.

Further in the cascade of potential activators, AICAR stimulates AMP-activated protein kinase, which affects energy homeostasis and may influence gene regulation. Forskolin, with its ability to elevate cAMP levels, activates protein kinase A, altering the activity of transcription factors and thereby gene expression profiles, including those related to proteins such as C2orf57. Resveratrol acts on sirtuins, modulating DNA repair and gene expression, possibly affecting the activity of proteins involved in these pathways. Additionally, Rapamycin, an mTOR pathway inhibitor, affects protein synthesis and gene expression, which may alter the functional state of proteins such as C2orf57. Small molecule inhibitors like SP600125, U0126, and LY294002 target specific kinases like JNK, MEK, and PI3K, respectively, each with the capacity to disrupt downstream signaling events. These disruptions can lead to changes in the transcription and activity of a range of proteins.

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