Staurosporine stands out as a potent kinase inhibitor with the capacity to impede phosphorylation events, a post-translational modification critical for the regulation of protein function. Similarly, LY294002 and its ability to inhibit PI3K interrupts the PI3K/AKT pathway, a central conduit for signals governing cell survival and metabolism. U0126 and PD98059, both targeting the MEK1/2 enzymes, along with ZM 336372's inhibition of RAF kinase, could alter the MAPK/ERK pathway, a pivotal route for cell proliferation and differentiation signals.
SB203580's specificity for p38 MAP kinase could attenuate the cellular response to stress and inflammation, while SP600125's inhibition of JNK might disrupt cellular apoptosis and survival mechanisms. Rapamycin, through its action on mTOR, may affect a multitude of processes from autophagy to protein synthesis. Cyclosporin A's role in inhibiting calcineurin perturbs the NFAT pathway, pivotal for immune response regulation. Bortezomib's proteasome inhibition can lead to an accumulation of proteins destined for degradation, thus affecting various cellular functions and stress responses. Thapsigargin's disruption of calcium homeostasis through SERCA inhibition can have widespread effects, given calcium's role as a ubiquitous second messenger. W-7, by antagonizing calmodulin, could impinge upon numerous proteins that rely on calmodulin for their activity, thus affecting calcium-dependent signaling processes.
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