Date published: 2025-11-24

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Junctophilin-2 Inhibitors

The chemical class of "Junctophilin-2 inhibitors" consists of compounds that indirectly modulate the function of Junctophilin-2 through various cellular mechanisms. Junctophilin-2 plays a significant role in the structural and functional organization of muscle cells by maintaining the close association of the plasma membrane with the sarcoplasmic or endoplasmic reticulum. The primary characteristic of these inhibitors is their indirect influence on Junctophilin-2 function by modulating calcium signaling and muscle cell physiology. Compounds like Dantrolene, Ryanodine, and Verapamil affect calcium release and influx, which are integral to Junctophilin-2's role in excitation-contraction coupling in muscle cells. By altering calcium dynamics, these compounds impact Junctophilin-2's function in maintaining junctional membrane complexes.

Another aspect of these inhibitors is their diverse nature and mechanisms of action. While some, such as Thapsigargin and Amlodipine, specifically target calcium handling mechanisms, others like Caffeine and Nifedipine alter calcium signaling more broadly. Additionally, compounds that influence membrane stability and ion channel function, such as Procaine and Chlorpromazine, can also indirectly affect Junctophilin-2's role in muscle cells. Furthermore, agents like Colchicine and Bepridil, which disrupt microtubule function and modulate calcium homeostasis, respectively, highlight the complex interplay between cellular structures and signaling pathways in regulating Junctophilin-2. In conclusion, the chemical class of "Junctophilin-2 inhibitors" includes a range of compounds that indirectly influence the function of Junctophilin-2. These inhibitors act through various mechanisms, including modulation of calcium signaling, alteration of ion channel function, and disruption of cellular structural organization. Their indirect mode of action reflects the intricate nature of Junctophilin-2's role in muscle cell physiology.

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