Compounds like Wortmannin and Triciribine can interfere with the PI3K/Akt pathway, which is central to the regulation of cell survival, proliferation, and metabolism. By inhibiting this pathway, these compounds can alter the cellular context in which LOC644477 operates. Ibrutinib and ZM 336372 target kinases involved in signal transduction pathways like BTK and RAF, respectively. Ibrutinib's effect on B-cell receptor signaling and ZM 336372's inhibition of the MAPK/ERK pathway can result in changes to the signaling landscape that may indirectly affect LOC644477.
Thapsigargin and PD 169316 affect calcium signaling and stress-related signaling, respectively. The former disrupts calcium homeostasis by inhibiting the SERCA pump, while the latter inhibits p38 MAPK, a key element in the cellular response to stress and inflammation. LY333531, by selectively inhibiting PKC-β, and Rapamycin, by targeting mTOR, can alter cellular processes such as cell cycle progression, angiogenesis, and autophagy, potentially influencing the function of LOC644477. SB431542 and Y-27632 affect signaling pathways involved in cell proliferation, differentiation, and the cytoskeleton. SB431542 inhibits TGF-beta signaling, while Y-27632 inhibits ROCK, which is involved in cytoskeleton organization. These inhibitors can shift the cellular environment and affect the activity of proteins linked to these pathways.
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