Date published: 2025-9-12

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FILIP Inhibitors

Chemical inhibitors of FILIP can act through various pathways to reduce its activity. LY294002 and Wortmannin are both PI3K inhibitors that block the PI3K/Akt signaling pathway, which is crucial for multiple cellular functions. When this pathway is inhibited, the phosphorylation and activity of downstream proteins, including FILIP, are decreased, leading to a reduction in FILIP's function within the cell. Similarly, PD98059 and U0126 specifically target MEK1/2, which are the upstream activators of ERK1/2, a part of the MAPK signaling pathway. The inhibition of MEK1/2 results in the decreased activation of ERK1/2 and thus lessens the phosphorylation of downstream targets, potentially including FILIP, which in turn inhibits FILIP's downstream signaling.

In parallel, other inhibitors like SB203580 and SP600125 target different MAPK pathways. SB203580 inhibits the p38 MAPK, while SP600125 acts upon the JNK pathway. By obstructing these pathways, the inhibitors can prevent the activation and function of proteins that are regulated by or act in conjunction with these kinases, which can include FILIP. This action results in the functional inhibition of FILIP's role in the cell. PP2, Dasatinib, and GF109203X are inhibitors that affect kinase signaling; PP2 and Dasatinib inhibit Src family kinases, and GF109203X inhibits protein kinase C (PKC). Src family kinases and PKC are integral to various signaling cascades, and their inhibition by these chemicals can lead to a reduction in FILIP activity due to the suppression of the related signaling pathways. Rapamycin, an mTOR inhibitor, disrupts the mTOR signaling pathway, which has wide-ranging effects on cell growth and proliferation. This disruption can lead to a decrease in the activity of proteins regulated by this pathway, including FILIP. Finally, Y-27632 and SB431542 inhibit the ROCK kinase and TGF-β receptor, respectively. The inhibition of ROCK kinase can affect the organization of the actin cytoskeleton and its associated signaling pathways, potentially leading to a decrease in FILIP activity. SB431542 hampers the SMAD signaling pathway activated by TGF-β receptors, which may be necessary for FILIP's full functionality, thereby inhibiting the protein's activity within the cell's signaling networks.

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