Date published: 2025-9-14

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TMEM141 Inhibitors

Cyclosporin A, by inhibiting calcineurin, affects calcium signaling, which is pivotal for numerous transmembrane proteins. Rapamycin, targeting the mTOR pathway, has implications for cellular growth and autophagy processes that transmembrane proteins can regulate or participate in. Staurosporine, with its broad kinase inhibition profile, may alter the phosphorylation landscape within the cell, impacting proteins involved in signal transduction. Brefeldin A disrupts protein trafficking by inhibiting ADP-ribosylation factors, potentially affecting the subcellular localization and hence the function of transmembrane proteins. U73122, by modulating the activity of phospholipase C, influences signaling cascades that can extend to the activity of transmembrane proteins. PD98059, which interferes with MEK in the MAPK/ERK pathway, could alter signaling routes that transmembrane proteins such as TMEM141 are part of, affecting their expression or function.

LY294002's inhibition of PI3K has downstream effects that may impact signaling pathways involving transmembrane proteins. Gö6976 affects protein kinase C, which is known to phosphorylate an array of proteins and could modify transmembrane protein functions accordingly. NF449 targets the Gs-alpha subunit of G-proteins, potentially altering GPCR-mediated signaling pathways that transmembrane proteins might engage with. Y-27632, as a ROCK inhibitor, would influence the cytoskeleton and possibly affect the mechanical aspects of transmembrane protein function. 2-APB modulates store-operated calcium entry, a process that is critical for calcium homeostasis and could be relevant for the function of calcium-sensitive transmembrane proteins. Lastly, Tunicamycin, by inhibiting N-linked glycosylation, could affect the stability and function of glycosylated transmembrane proteins.

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