Date published: 2026-4-8

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Mucin 11/12 Inhibitors

Chemical inhibitors of Mucin 11/12 can exert their inhibitory effects through various mechanisms that disrupt the protein's maturation, secretion, and functional expression. Phosphoramidon targets metalloproteases that are instrumental in the shedding of Mucin 11/12, ensuring that the protein remains bound to the cell surface and is functionally inhibited. GW4869, by inhibiting neutral sphingomyelinase, hampers the formation of ceramide, a critical molecule for Mucin 11/12's secretion in exosomes, thereby preventing its functional activity. Brefeldin A and Monensin both disrupt the Golgi apparatus, a critical site for Mucin 11/12's glycosylation. By doing so, they inhibit the protein's proper processing and maturation, which is essential for its function. Swainsonine and Castanospermine specifically target the glycosylation process: Swainsonine inhibits alpha-mannosidase II, leading to under-glycosylation of Mucin 11/12, and Castanospermine inhibits glucosidase, preventing proper folding and trafficking, both resulting in the inhibition of Mucin 11/12's functional form.

Tunicamycin contributes to the inhibition of Mucin 11/12 by blocking N-linked glycosylation, critical for the protein's stability and folding, thereby preventing it from attaining a functional state. Bay 11-7082 indirectly inhibits Mucin 11/12 by inhibiting NF-κB activation, a key regulator in mucin gene expression, thus reducing the production of Mucin 11/12 at the transcription level. PD98059 and SB203580 target MAPK pathways; PD98059 inhibits MEK in the MAPK/ERK pathway, and SB203580 inhibits p38 MAPK, both of which are important for the regulation of Mucin 11/12 synthesis and secretion. LY294002 disrupts PI3K, which is critical for the synthesis and secretion signaling of Mucin 11/12, leading to the inhibition of these processes. Lastly, Genistein inhibits tyrosine kinases that phosphorylate proteins in the signaling pathways responsible for mucin production, including Mucin 11/12, thereby inhibiting its functional activity.

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