Date published: 2025-11-3

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LOC391359 Inhibitors

Staurosporine is a robust kinase inhibitor, adept at suppressing a multitude of kinases that could be responsible for the phosphorylation of LOC391359, thereby potentially reducing its activity. In parallel, Rapamycin, by targeting mTOR, alters the signaling pathways essential for the function or expression of LOC391359, assuming there is an association between them. LY294002 takes aim at PI3K, which could lead to a decrease in Akt signaling, influencing LOC391359's activity if it is part of the PI3K/Akt pathway. Similarly, PD98059 and U0126, both of which inhibit MEK, could lead to a decrease in the MAPK/ERK pathway activity, which would affect LOC391359's role if it is a component of this signal transduction pathway.

The p38 MAPK pathway, an avenue for transducing cellular stress signals, is targeted by SB203580, which could modify LOC391359 activity if the protein responds to such signals. SP600125 operates by inhibiting JNK, which could likewise recalibrate LOC391359's function if it is involved in the JNK signaling cascade. Bortezomib disrupts normal proteasomal activity, leading to an accumulation of proteins and potentially stabilizing LOC391359 if it is usually marked for degradation. Conversely, 17-AAG antagonizes Hsp90, which could destabilize LOC391359 should it depend on Hsp90 for its folding or stability. Thapsigargin, by impeding SERCA, affects calcium homeostasis, which could influence LOC391359 if it is calcium-sensitive. Cyclopamine, which hampers the Hedgehog signaling pathway, could recalibrate LOC391359's activity if it is intertwined with this pathway. Lastly, Imatinib, by targeting specific tyrosine kinases, could alter the phosphorylation status and thereby the activity of LOC391359, provided there is a connection between them.

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