Date published: 2025-9-14

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LOC646237 Inhibitors

Staurosporine operates as a kinase inhibitor with a broad target spectrum, capable of modulating a multitude of kinases that could be implicated in the regulation or activation of LOC646237. Its inhibitory effects span across various kinase-dependent signaling pathways that are pivotal in cellular homeostasis and function. In parallel, SB203580's inhibition of p38 MAP kinase and U0126's suppression of MEK1/2 specifically target the MAPK/ERK pathway. By impeding these kinases, both compounds serve to dampen the biochemical dialog that may dictate the behavior of LOC646237, effectively reducing its participation in cellular processes.

LY294002, by curtailing PI3K activity, influences the PI3K/AKT pathway, known for its role in a wide array of cellular functions, including growth, survival, and metabolism. The regulation exerted by this inhibitor can extend to proteins that are regulated by or responsive to PI3K/AKT signaling, such as LOC646237. Bortezomib's role as a proteasome inhibitor introduces another dimension to the regulatory control by impacting protein degradation pathways. This alteration can affect the stability and turnover of proteins, including LOC646237, thus modulating its cellular concentration and function. Alsterpaullone and PD0325901, both inhibitors of cyclin-dependent kinases and MEK, respectively, assert control over cell cycle progression and ERK phosphorylation. These inhibitors can exert influence on LOC646237 if it is implicated in cell cycle regulation or if its activity is modulated by ERK signaling. The JNK pathway, targeted by SP600125, and Hsp90, targeted by 17-AAG, are further examples where the inhibition can affect transcription factor activity and protein folding, which may alter the functional landscape of LOC646237.

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