Date published: 2025-9-22

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2700049P18Rik Inhibitors

Chemical inhibitors of 2700049P18Rik can exert their effects through various mechanisms by targeting specific pathways and enzymes that are crucial for the protein's functional activity. Staurosporine acts as a broad-spectrum protein kinase inhibitor, and by doing so, it can prevent vital phosphorylation events necessary for the functional activity of 2700049P18Rik. Similarly, wortmannin and LY294002 are both inhibitors of phosphatidylinositol 3-kinase (PI3K), an enzyme that regulates numerous signaling pathways; their inhibition can disrupt downstream signals essential for 2700049P18Rik function. Rapamycin, by inhibiting mTOR, a central cell growth regulator, can lead to the inhibition of 2700049P18Rik if its function is connected to mTOR signaling pathways. U0126, PD98059, and SB203580 specifically inhibit key components of the MAPK pathway, namely MEK1/2 and p38 MAP kinase, which can result in the inhibition of 2700049P18Rik if it relies on this pathway for activation or regulation.

Further, SP600125 targets c-Jun N-terminal kinase, which can impair signaling pathways that 2700049P18Rik utilizes, while ZM-447439, an Aurora kinase inhibitor, has the potential to disrupt cell division processes involving 2700049P18Rik. PP2, by inhibiting Src family tyrosine kinases, can affect the Src kinase-related signaling pathways, potentially necessary for 2700049P18Rik's activity. Bortezomib, as a proteasome inhibitor, can affect the degradation process of proteins and inhibit the function of 2700049P18Rik if it is involved in proteasomal pathways. Lastly, thapsigargin impairs the sarco/endoplasmic reticulum Ca2+-ATPase, which can inhibit 2700049P18Rik by interfering with calcium-dependent signaling that the protein might be part of. Each of these chemicals, by targeting specific enzymes or pathways, can lead to the functional inhibition of 2700049P18Rik within the cellular context, providing a diverse set of tools for dissecting the protein's role and regulation mechanisms.

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