Date published: 2025-9-15

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C9orf117 Activators

Forskolin stands out for its ability to boost cAMP levels, which in turn activates PKA, a kinase that can phosphorylate a variety of substrates including transcription factors that regulate gene expression, potentially upregulating C9orf117. Similarly, IBMX acts to maintain elevated cAMP levels by inhibiting phosphodiesterases, thereby extending the duration of PKA-mediated signaling which could enhance C9orf117 expression. Compounds like PMA activate protein kinase C (PKC), which is involved in numerous cellular processes, including the regulation of gene expression. This activation could initiate signaling cascades that modulate C9orf117 activity. Ionomycin, by increasing intracellular calcium, can trigger calcium-dependent proteins and pathways, possibly affecting C9orf117 expression.

Epigenetic modifiers, such as 5-Azacytidine and Trichostatin A (TSA), change the epigenetic landscape of the cell, leading to a more transcriptionally active chromatin structure and potentially increasing the expression of genes like C9orf117. Retinoic acid, by binding to its nuclear receptors, has a profound impact on gene regulation, which might include C9orf117. Flavonoids such as Epigallocatechin gallate (EGCG) exert their influence through interactions with various signaling molecules and pathways, which can affect C9orf117. Meanwhile, Sodium butyrate, another histone deacetylase inhibitor, can induce chromatin changes that may lead to upregulation of C9orf117 expression. Inhibitors of key signaling kinases, like LY294002 for PI3K, PD98059 for MEK, and SP600125 for JNK, alter the dynamics of their respective pathways, impacting a myriad of cellular functions including the regulation of transcription factors and genes, potentially influencing C9orf117 expression.

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