Date published: 2025-9-11

00800 4573 8000

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REEP3 Inibitori

I comuni inibitori di REEP3 includono, ma non solo, Brefeldin A CAS 20350-15-6, Monensin A CAS 17090-79-8, Nocodazolo CAS 31430-18-9, Taxol CAS 33069-62-4 e Colchicina CAS 64-86-8.

Inhibitors of REEP3 include a number of different compounds that interfere with various biological processes critical to the protein's function. Compounds that destabilize or stabilize microtubules can indirectly inhibit REEP3 by altering its ability to modulate microtubule dynamics, which is critical for its role in microtubule-dependent processes. For example, the action of microtubule-stabilizing agents can disrupt the delicate balance required for REEP3 to exert its effect on the microtubule network, while microtubule-destabilizing agents can prevent REEP3 from interacting with microtubules, impairing their functionality. Similarly, disruption of actin filaments by some compounds could impact the cytoskeletal interactions of REEP3, which are integral to the cell morphology and membrane trafficking processes that REEP3 regulates. In addition, inhibition of key GTPases involved in vesicle cleavage and cytoskeletal organization may influence the role of REEP3 in membrane remodeling and dynamics.

In addition, inhibitors that target vesicle trafficking and Golgi function may also indirectly lead to a reduction in REEP3 activity. By disrupting the function of small GTPases central to vesicle trafficking, such as ARF, or by inhibiting Golgi-related proteins, these compounds may interfere with REEP3 involvement in endoplasmic reticulum membrane shaping and trafficking between the ER and Golgi. In addition, inhibition of enzymes responsible for post-translational modifications, such as glycosylation, may affect the stability and proper function of REEP3, preventing its proper folding and trafficking within the ER.

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