Date published: 2025-9-10

021-6093-6350

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ACOT11 抑制因子

Chemical inhibitors of ACOT1 include a range of compounds that exert inhibitory effects through various mechanisms. Trifluoperazine, W-7 Hydrochloride, Ophiobolin A, Chlorpromazine, Thioridazine, and R24571 are all calmodulin antagonists that inhibit ACOT1 by blocking the calcium/calmodulin-dependent pathways required for its optimal enzymatic activity. These inhibitors work by impeding the interaction between calmodulin and ACOT1, which is essential for the regulation of ACOT1's function in lipid metabolism. By disrupting this interaction, these chemicals effectively reduce the activity of ACOT1, leading to decreased fatty acid hydrolysis.

Additionally, chemicals such as Phenoxybenzamine and Methylene Blue inhibit ACOT1 indirectly. Phenoxybenzamine does so by antagonizing adrenergic receptors, leading to alterations in lipid metabolism that result in reduced ACOT1 activity. Methylene Blue, on the other hand, influences the redox state of cells, which can alter the cofactor availability or oxidation state required for ACOT1's function. Genistein and Bisindolylmaleimide I inhibit ACOT1 by targeting phosphorylation events. Genistein, as a tyrosine kinase inhibitor, disrupts phosphorylation-dependent regulatory mechanisms of ACOT1, while Bisindolylmaleimide I, a protein kinase C inhibitor, alters the phosphorylation status of proteins that regulate ACOT1's role in lipid metabolism. Quercetin, another kinase inhibitor, interferes with kinase-mediated signaling pathways that are crucial for ACOT1's enzymatic activity. Lastly, LY294002 inhibits ACOT1 by disrupting insulin signaling-dependent lipid metabolism pathways, impacting the role of ACOT1 in fatty acid hydrolysis. Each of these chemicals, through their respective mechanisms, achieves the inhibition of ACOT1 by altering the biochemical and cellular pathways that govern its activity.

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产品名称CAS #产品编号数量价格应用排名

LY 294002

154447-36-6sc-201426
sc-201426A
5 mg
25 mg
¥1365.00
¥4423.00
148
(1)

LY294002 是一种 PI3K 抑制剂,它可能会通过破坏依赖于胰岛素信号的脂质代谢途径来抑制 ACOT1,在这些途径中,ACOT1 在脂肪酸水解中发挥作用。