Date published: 2025-9-15

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TMEM178 Inhibitors

TMEM178 inhibitors, as presented here, are primarily focused on chemicals that indirectly affect the function or signaling pathways associated with TMEM178. This protein is involved in cellular processes such as calcium signaling, autophagy, and immune response modulation, and its direct inhibitors are not well-established in the current scientific literature. The inhibitors listed target various key pathways and enzymes that are either upstream or downstream of TMEM178, thereby providing a range of possibilities for indirect inhibition. The inhibitors include proteasome inhibitors like Bortezomib, which disrupt the protein degradation pathway, potentially affecting proteins that regulate or interact with TMEM178. Calcium homeostasis is another critical aspect, with Thapsigargin acting as a potent SERCA pump inhibitor, thereby influencing calcium signaling pathways linked to TMEM178. Glycosylation processes are targeted by Tunicamycin, affecting the maturation and function of proteins associated with TMEM178. The mTOR pathway, a central regulator of cell growth and autophagy, is targeted by inhibitors like Rapamycin, indirectly impacting TMEM178-associated pathways.

Immunosuppressants such as Cyclosporin A and FK-506 inhibit calcineurin, a protein phosphatase involved in immune response and potentially linked to TMEM178 signaling. Autophagy, a process that TMEM178 might influence, is targeted by Chloroquine, an autophagy inhibitor. The PI3K/Akt pathway, a critical signaling pathway in many cellular processes, is inhibited by compounds like LY 294002 and Wortmannin, potentially affecting TMEM178-related signaling. Furthermore, inhibitors targeting the MAPK/ERK pathway (U0126), the JNK pathway (SP600125), and the p38 MAPK pathway (SB 203580) are included, considering their broad impact on cellular signaling processes that could intersect with TMEM178 functions.

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