FNDC8 inhibitors work through a diverse set of biochemical routes to influence the protein's activity and stability. Rapamycin, for instance, disrupts the mTOR pathway, specifically targeting both mTORC1 and mTORC2 complexes. These complexes phosphorylate substrates that are crucial for FNDC8 function, hence their inhibition leads to reduced FNDC8 activity. Similarly, LY294002 acts as a PI3K inhibitor, which in turn suppresses Akt activation, an element of the PI3K-Akt-mTOR signaling axis that influences FNDC8 protein stability. PD98059 is a MEK inhibitor affecting the Ras/Raf/MEK/ERK pathway. By inhibiting MEK1, it disables an upstream kinase of ERK that has a direct interaction with FNDC8, thus altering its functionality.
Further into the realm of kinase inhibitors, Imatinib targets tyrosine kinases like c-ABL, c-KIT, and PDGFR, resulting in diminished FNDC8 expression levels. SB431542 specifically inhibits TGF-β, thereby disrupting the SMAD pathway, which interacts with FNDC8 for functional regulation. NSC23766 is a Rac1 inhibitor affecting the Rho family of GTPases that plays a role in cytoskeletal dynamics, which in turn influences FNDC8's functional association with membrane structures. These chemical inhibitors illustrate how complex the regulation of FNDC8 is, being susceptible to influences from various biochemical pathways. Each inhibitor acts on a different biochemical mechanism, cumulatively covering a broad range of FNDC8 functional aspects without unwanted broader cellular implications.
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