Date published: 2025-10-31

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C2orf18 Inhibitors

Chemical inhibitors of C2orf18 target various signaling pathways and molecular mechanisms to achieve functional inhibition. Genistein and Dasatinib work by inhibiting tyrosine kinases, which are essential for the signal transduction that C2orf18 relies upon for its activity. The inhibition of these kinases prevents the phosphorylation events that are crucial for C2orf18 to carry out its functions. Similarly, Erlotinib and Gefitinib directly inhibit the activity of EGFR tyrosine kinase, a key signaling molecule that may be involved in pathways utilized by C2orf18. By blocking EGFR, these inhibitors can disrupt the signaling cascade, leading to a decrease in C2orf18 activity.

Furthermore, PI3K inhibitors such as PIK-75, IC-87114, and LY294002 prevent the phosphorylation and subsequent activation of AKT, a serine/threonine-specific protein kinase that plays a role in multiple cellular processes including those that involve C2orf18. By impeding this pathway, these inhibitors can reduce the functional activity of C2orf18. Additionally, the inhibition of other kinases like p38 MAP kinase by SB203580, MEK1/2 by PD98059, and JNK by SP600125 can lead to a reduction in the functional activity of C2orf18 due to their roles in the regulation and function of proteins within their respective pathways. The mTOR pathway, involved in protein synthesis and cell growth, can also be inhibited by compounds such as Rapamycin. By binding to mTOR and inhibiting its function, Rapamycin can suppress the activation of proteins downstream, including C2orf18. Lastly, PP2 disrupts Src family kinases, which are involved in various signaling pathways that C2orf18 may be a part of, leading to the inhibition of its function. By targeting these specific kinases and pathways, the aforementioned inhibitors can effectively reduce the functional activity of C2orf18.

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