LY294002, as a PI3K inhibitor, suppresses the PI3K/AKT pathway, a signaling cascade that is pivotal for numerous cellular functions including growth, proliferation, and survival, hence can indirectly influence the activity of LOC730229. Rapamycin, an inhibitor of mTOR, can have far-reaching effects on cellular metabolism and growth signals that may intersect with LOC730229's function or expression. U0126 and SB203580, by specifically targeting the MEK1/2 and p38 MAPK respectively, can alter the MAPK/ERK pathway and the cellular stress response, which are often involved in the regulation of various proteins, including LOC730229. Cyclopamine and itraconazole can inhibit the Hedgehog signaling pathway, potentially altering cell fate and growth patterns that can indirectly affect the function of LOC730229.
Bortezomib acts on the proteasome, a complex responsible for protein degradation, which can influence the turnover and therefore the levels of LOC730229 within cells. Chelerythrine, by inhibiting PKC, can modify signal transduction that may regulate LOC730229. Similarly, SP600125 as a JNK inhibitor can interfere with the JNK signaling pathway, which can modulate the activity of LOC730229. W7, through its antagonistic action on calmodulin, disrupts calcium signaling, a universal cellular messenger system that can impinge upon the function of LOC730229. Lastly, imatinib, which targets specific tyrosine kinases, can have a broad impact on cell signaling, potentially modifying the activity of LOC730229 via effects on BCR-ABL, c-KIT, and PDGF receptors.
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