LY294002 and Wortmannin, for example, are both inhibitors of PI3K, an upstream regulator of Akt signaling, which is a pivotal pathway for cell survival and metabolism. By inhibiting PI3K, these compounds can reduce the activity of Akt, thereby affecting any regulatory roles LOC728991 may have in this pathway. Rapamycin, targeting mTOR, can have a broad effect on cell growth and proliferation, processes in which LOC728991 may be implicated. SB203580 and PD98059, as well as U0126, are inhibitors of the MAPK family of enzymes, which are involved in cell differentiation, proliferation, and stress response signaling. The inhibition of these kinases can therefore impact LOC728991's activity if it is a part of these signaling pathways.
PP2 disrupts Src kinase signaling, which affects cell adhesion and survival, while KN-93, by inhibiting CaMKII, affects calcium signaling, which is integral to numerous cellular processes including those that LOC728991 may influence. PD173074 targets FGFR signaling, thereby affecting cell growth and development, which could alter LOC728991's function if it is involved in these processes. SP600125 inhibits JNK, which is involved in controlling apoptosis and inflammatory responses, processes where LOC728991 may play a regulatory role. ZM-447439 inhibits Aurora kinases, which are essential for mitotic progression, potentially altering LOC728991's activity if it is involved in cell division. Lastly, Olaparib, a PARP inhibitor, affects the DNA damage response, and by doing so, can influence LOC728991's function in genomic stability and repair mechanisms.
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