Date published: 2025-9-12

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GOLGA6A-D Inhibitors

GOLGA6A-D inhibitors encompass a diverse range of chemical compounds that impact various cellular mechanisms leading to the downregulation of GOLGA6A-D activity. Wortmannin and Brefeldin A are prominent examples, where Wortmannin's inhibition of PI3K activity leads to a subsequent decrease in AKT signaling that is crucial for Golgi apparatus function, thereby indirectly affecting GOLGA6A-D. Brefeldin A's mechanism is different; it disrupts the Golgi structure by inhibiting ARF, which is essential for vesicle formation, and this disturbance in Golgi organization can result in an indirect inhibition of GOLGA6A-D. Similarly, the inhibition of dynamin by Dynasore and GBF1 by Golgicide A disrupts key trafficking events and Golgi structure maintenance, respectively, revealing how intracellular transport processes are crucial for GOLGA6A-D functionality. Monensin's alteration of intracellular pH and cation homeostasis leads to Golgi dysfunction, and as GOLGA6A-D is implicated in Golgi processes, its activity is consequently hindered. Nocodazole and Vinblastine impact microtubule dynamics, which are integral to Golgi positioning and function, thereby indirectly reducing GOLGA6A-D activity due to the disruption of this cellular framework.

The manipulation of the cytoskeleton also plays a significant role in the inhibition of GOLGA6A-D, as demonstrated by Cytochalasin D, which compromises actin filament formation and thereby potentially impairs GOLGA6A-D associated with the Golgi apparatus. Tunicamycin introduces ER stress by blocking N-linked glycosylation, which can cascade down to the Golgi apparatus, impacting GOLGA6A-D's role in its functioning. Ilomastat's inhibition of extracellular matrix remodeling can perturb cellular signaling, indirectly influencing GOLGA6A-D. Moreover, Betulinic Acid and Swainsonine target apoptosis and glycoprotein processing within the Golgi, respectively, which can lead to a breakdown in Golgi structure and function, and by extension, an indirect inhibition of GOLGA6A-D activity. Each of these inhibitors, through their specific actions on different pathways and cellular structures, contributes to the overall reduction in GOLGA6A-D functionality by interrupting the delicate balance of processes it is involved in.

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