Date published: 2025-9-5

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C3orf72 Inhibitors

The chemical class denoted as C3orf72 Inhibitors encompasses a collection of compounds strategically chosen to modulate signaling pathways associated with the C3orf72 protein. Metformin, a well-known antidiabetic drug, activates AMP-activated protein kinase (AMPK), which plays a role in cellular energy homeostasis and can potentially influence C3orf72 activity. Forskolin activates adenylate cyclase, leading to increased cAMP levels, a potential modulator of C3orf72 signaling pathways.

AICAR (Acadesine) activates AMPK, contributing to cellular energy homeostasis, providing another avenue for potential modulation of C3orf72. GW501516 (Cardarine) activates PPARδ, influencing metabolic pathways that might intersect with C3orf72 function. LY294002 inhibits PI3-kinase, disrupting the PI3K/AKT signaling axis, which can potentially affect C3orf72 signaling. Rapamycin, an mTOR inhibitor, disrupts mTOR-dependent cellular events, providing another potential avenue for modulation. SB216763 is a GSK-3 inhibitor, impacting the Wnt/β-catenin signaling pathway, which could be linked to C3orf72. A-769662, another AMPK activator, can contribute to cellular energy homeostasis, potentially influencing C3orf72 activity. Rosiglitazone activates PPARγ, influencing transcriptional regulation that may intersect with C3orf72. PD98059 selectively inhibits MEK1, disrupting the MAPK pathway, which could be involved in C3orf72 signaling. SB431542 inhibits the TGF-β type I receptor, modulating the TGF-β pathway, providing another potential avenue for C3orf72 modulation. U0126 blocks MEK1 and MEK2, key kinases in the MAPK signaling cascade, potentially influencing C3orf72 regulation. Collectively, these compounds offer a diverse toolkit for investigating the modulation of cellular processes associated with C3orf72, even in the absence of direct inhibitors, by targeting key pathways involved in its regulation.

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