Date published: 2025-9-13

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PBR Inhibitors

The chemical class of PBR Inhibitors encompasses a range of compounds that indirectly affect the functionality of PBR, a protein involved in a variety of cellular processes including cholesterol transport, steroidogenesis, and mitochondrial functions. These inhibitors operate through various mechanisms, focusing on modulating the cellular pathways that influence PBR activity. Key to this class are compounds like PK11195 and Ro5-4864, which, despite being ligands for PBR, exhibit antagonist-like effects on the receptor, inhibiting its functional role in processes like steroidogenesis and mitochondrial regulation. Benzodiazepine derivatives such as Diclazepam and antagonists like Flumazenil modulate GABAergic signaling, which is intricately connected to PBR's function in neurosteroidogenesis and stress responses. Antifungal agents like Clotrimazole, Ketoconazole, and Itraconazole inhibit cytochrome P450 enzymes, impacting steroid biosynthesis pathways in which PBR plays a crucial role. By altering these pathways, these compounds can indirectly modulate PBR activity.Glucocorticoid receptor antagonists such as Mifepristone influence pathways involved in stress response and inflammation, affecting PBR's role in these processes. Similarly, calcium channel blockers like Amlodipine, Verapamil, Nitrendipine, and Diltiazem can indirectly influence PBR activity by modulating calcium signaling pathways that are linked to cellular processes such as apoptosis and mitochondrial function. Overall, the PBR Inhibitors class represents a diverse array of chemical compounds that, through their influence on various signaling pathways and cellular processes, can indirectly inhibit the activity of PBR. While these compounds do not interact directly with PBR, their role in modulating the cellular environment and influencing key pathways such as GABAergic signaling, steroid biosynthesis, and calcium-dependent processes contributes to the inhibition of PBR's functionality in maintaining cellular homeostasis. Understanding the impact of these inhibitors on PBR and the broader cellular functions it influences is crucial for comprehending the complex interplay between cellular signaling, steroidogenesis, and mitochondrial functions.

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