Date published: 2025-9-14

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CYP2B1 Inhibitors

The chemical class of CYP2B1 inhibitors encompasses a range of compounds that indirectly modulate the activity of the CYP2B1 enzyme. These compounds are characterized by their ability to interact with the cytochrome P450 system, either through competitive inhibition, allosteric modulation, or affecting the enzymes expression. Their primary mechanism is not the direct inhibition of CYP2B1 but rather an influence on the broader cytochrome P450 system within which CYP2B1 operates. Compounds such as Ketoconazole, Quinidine, Ticlopidine, Clotrimazole, and Chloramphenicol are known to inhibit multiple cytochrome P450 enzymes, including CYP2B1. Their broad-spectrum activity on the cytochrome P450 system suggests that these compounds can reduce the metabolic capacity of CYP2B1. For example, Ketoconazole and Clotrimazole are potent inhibitors of several P450 enzymes, thus they could indirectly affect the functioning of CYP2B1 through competitive inhibition or by altering its metabolic pathway.Other compounds in this class, including Clopidogrel, Sulfaphenazole, Omeprazole, Montelukast, Fluoxetine, and Sertraline, exhibit varying degrees of inhibition on different cytochrome P450 enzymes. While some of these compounds primarily target enzymes like CYP2C9 or CYP2C19, their influence on CYP2B1 can stem from overlapping substrate specificities or through modulation of liver enzyme expression. For instance, Omeprazole, while primarily inhibiting CYP2C19, can affect CYP2B1 due to its role in the metabolism of similar substrates. Additionally, certain drugs like Phenobarbital, known for inducing various cytochrome P450 enzymes, can also exhibit competitive inhibition under specific conditions, impacting CYP2B1 activity. These drugs demonstrate the complex interplay within the cytochrome P450 system, where induction and inhibition can coexist, influencing the metabolic activity of specific enzymes like CYP2B1.

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