Date published: 2025-11-7

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C17orf67 Activators

Dibutyryl-cAMP, a synthetic analog of cAMP, permeates cell membranes to activate protein kinase A, which could signal to pathways that include C17orf67. Epidermal Growth Factor, by engaging with tyrosine kinase receptors, sets off a cascade of intracellular signaling that may intersect with processes involving C17orf67. Proteasome inhibitor MG132 alters the degradation pathways, potentially leading to the increased stability and presence of C17orf67 within the cell. Similarly, Lithium chloride acts by inhibiting GSK-3, a kinase within the Wnt signaling pathway, thereby potentially impacting the activity of C17orf67. Retinoic Acid is known for its profound impact on gene expression, which may include the upregulation of C17orf67.

Further affecting gene regulation, Genistein and Sodium Butyrate act as a tyrosine kinase inhibitor and a histone deacetylase inhibitor, respectively. These actions can alter transcriptional landscapes, leading to changes in the levels and activity of various proteins, including C17orf67. LY294002, by inhibiting PI3K, and PD98059, by inhibiting MEK1/2, modulate critical cellular pathways like AKT and MAPK/ERK, which are extensive networks capable of influencing a broad array of proteins, possibly including C17orf67. Moreover, 2-Deoxy-D-glucose's inhibition of glycolysis may affect cellular energy balance, which can lead to a cellular state that indirectly influences the activity of C17orf67. Inhibitors such as SB203580 and Roscovitine target p38 MAPK and cyclin-dependent kinases, respectively, impacting stress response pathways and cell cycle regulation, which are critical processes that might affect C17orf67 activity.

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