Date published: 2025-11-2

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UBXN2B Activators

UBXN2B activators compose a diverse set of chemicals, predominantly focused on modulating proteostasis and protein degradation pathways. Central to this group is MG-132, a renowned proteasome. By blocking proteasomal function, MG-132 can shift the equilibrium of protein degradation, which in turn, may indirectly affect the dynamics of UBXN2B within the cell. ALLN and Lactacystin, sharing similar actions on proteases, weave into this narrative, underscoring the importance of proteostasis in influencing UBXN2B's cellular role.

Another critical player in this panorama is Eeyarestatin I. With its effect on endoplasmic reticulum-associated degradation, it bridges the intracellular conversation between the ER and ubiquitin-proteasome system, indirectly drawing UBXN2B into the fold. MLN4924, by inhibiting the NEDD8-activating enzyme, paints another facet of ubiquitination, suggesting that altered ubiquitin dynamics can resonate with UBXN2B's function. The broad-acting agent, Curcumin, and lysosomal enzyme, Chloroquine, illustrate the vast cellular landscape these activators can touch upon. Both Bortezomib and Withaferin A, each with its unique method of influencing protein aggregation and degradation, underline the intricate balance of cellular proteostasis and its ties to UBXN2B's action. The list culminates with Concanamycin A, emphasizing that influencing broader cellular mechanisms like V-ATPase function can cascade down to specific proteins like UBXN2B.

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