TRAPPC10 Inhibitors
The chemical class known as TRAPPC10 Inhibitors refers to a diverse group of compounds that indirectly inhibit the activity of the TRAPPC10 protein. These chemicals are not directly antagonistic to TRAPPC10 but instead modulate various cellular mechanisms and signaling pathways that are essential for the proper functioning of TRAPPC10 within the cell. For example, Brefeldin A and Golgicide A target the secretory pathway between the endoplasmic reticulum and the Golgi apparatus, a pathway that is crucial for the transport and sorting of proteins and lipids in which TRAPPC10 plays a role. Disruption of this pathway can lead to a cascade of effects that ultimately impair the function of TRAPPC10.
Additionally, other compounds such as Monensin, Nocodazole, and Paclitaxel act on the cytoskeletal components of the cell, like microtubules, which are vital for vesicular transport. These agents can lead to either stabilization or destabilization of microtubules, resulting in the disruption of vesicular trafficking and indirectly impacting TRAPPC10's role in these processes. Similarly, Cytochalasin D and Wiskostatin disrupt actin filaments, affecting cellular dynamics and potentially the vesicle formation and movement where TRAPPC10 is implicated. Agents like Tunicamycin induce stress in the endoplasmic reticulum by inhibiting glycosylation, a modification necessary for many proteins that travel through the secretory pathway, where TRAPPC10 is involved. Furthermore, Betulinic acid and Genistein can alter cellular pathways through their action on multiple targets, including those that may intersect with the trafficking pathways regulated by TRAPPC10.
Items 1 to 10 of 12 total
Display:
| Product Name | CAS # | Catalog # | QUANTITY | Price | Citations | RATING |
|---|---|---|---|---|---|---|
Brefeldin A | 20350-15-6 | sc-200861C sc-200861 sc-200861A sc-200861B | 1 mg 5 mg 25 mg 100 mg | $30.00 $52.00 $122.00 $367.00 | 25 | |
Disrupts transport between the endoplasmic reticulum and Golgi apparatus, possibly affecting TRAPPC10 function. | ||||||
Monensin A | 17090-79-8 | sc-362032 sc-362032A | 5 mg 25 mg | $152.00 $515.00 | ||
Alters Golgi apparatus function, which can indirectly influence TRAPPC10’s role in trafficking. | ||||||
Nocodazole | 31430-18-9 | sc-3518B sc-3518 sc-3518C sc-3518A | 5 mg 10 mg 25 mg 50 mg | $58.00 $83.00 $140.00 $242.00 | 38 | |
Destabilizes microtubules, potentially impacting vesicular transport processes involving TRAPPC10. | ||||||
Taxol | 33069-62-4 | sc-201439D sc-201439 sc-201439A sc-201439E sc-201439B sc-201439C | 1 mg 5 mg 25 mg 100 mg 250 mg 1 g | $40.00 $73.00 $217.00 $242.00 $724.00 $1196.00 | 39 | |
Stabilizes microtubules and can disrupt normal trafficking mechanisms that TRAPPC10 may be involved in. | ||||||
Colchicine | 64-86-8 | sc-203005 sc-203005A sc-203005B sc-203005C sc-203005D sc-203005E | 1 g 5 g 50 g 100 g 500 g 1 kg | $98.00 $315.00 $2244.00 $4396.00 $17850.00 $34068.00 | 3 | |
Inhibits microtubule polymerization, which can affect TRAPPC10-related vesicle transport. | ||||||
Cytochalasin D | 22144-77-0 | sc-201442 sc-201442A | 1 mg 5 mg | $145.00 $442.00 | 64 | |
Disrupts actin filament organization, which can alter trafficking pathways regulated by TRAPPC10. | ||||||
Dynamin Inhibitor I, Dynasore | 304448-55-3 | sc-202592 | 10 mg | $87.00 | 44 | |
Inhibits dynamin, potentially influencing vesicular release and trafficking where TRAPPC10 functions. | ||||||
Epoxomicin | 134381-21-8 | sc-201298C sc-201298 sc-201298A sc-201298B | 50 µg 100 µg 250 µg 500 µg | $134.00 $215.00 $440.00 $496.00 | 19 | |
Targets the Golgi apparatus, potentially disrupting processes where TRAPPC10 is involved. | ||||||
Tunicamycin | 11089-65-9 | sc-3506A sc-3506 | 5 mg 10 mg | $169.00 $299.00 | 66 | |
Induces ER stress by inhibiting N-linked glycosylation, possibly affecting TRAPPC10’s trafficking role. | ||||||
Betulinic Acid | 472-15-1 | sc-200132 sc-200132A | 25 mg 100 mg | $115.00 $337.00 | 3 | |
Alters multiple cellular pathways, including those that may affect TRAPPC10-mediated trafficking. | ||||||