Date published: 2025-9-22

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CEL Inhibitors

Carboxylesterase-like (CEL) inhibitors are a class of chemical compounds that target and inhibit the activity of enzymes within the carboxylesterase family, particularly those resembling carboxylesterase-like enzymes. Carboxylesterases are a group of enzymes that catalyze the hydrolysis of ester bonds in various substrates, ranging from small molecules to complex lipids. CEL inhibitors function by binding to the active site of these enzymes, thereby blocking their catalytic activity. The inhibition mechanism can vary, involving either competitive inhibition, where the inhibitor competes with the substrate for the active site, or non-competitive inhibition, where the inhibitor binds to a different site on the enzyme, altering its conformation and reducing its activity. The chemical structure of CEL inhibitors is diverse, often featuring specific functional groups that interact with key amino acids in the enzyme's active site. These interactions typically include hydrogen bonding, hydrophobic interactions, and, in some cases, covalent bonding with the enzyme's active serine residue. The study and design of CEL inhibitors are significant in the context of understanding enzyme-substrate interactions and the broader implications of enzyme inhibition in biochemical pathways. By inhibiting CEL enzymes, researchers can elucidate the role these enzymes play in metabolic processes, including lipid metabolism and the breakdown of complex molecules. Furthermore, CEL inhibitors are often employed as tools in biochemical assays to study the kinetics and structural biology of carboxylesterases, providing insights into enzyme function, substrate specificity, and the structural basis of enzyme activity. The design of these inhibitors typically involves a thorough understanding of the enzyme's structure through techniques like X-ray crystallography or molecular modeling, which allows for the identification of key binding sites and the development of molecules with high specificity and potency.

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