Date published: 2025-9-13

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4930511I11Rik Inhibitors

Armc12 Inhibitors encompass a range of chemical compounds that indirectly modulate the cellular and molecular context in which ARMC12 operates. The chemicals listed target various signaling pathways and cellular processes, which, when altered, can influence the activity and function of ARMC12 by extension. For instance, Cyclopamine's ability to inhibit the Hedgehog signaling pathway can result in downstream effects on cellular processes related to proliferation and differentiation, where ARMC12 may be implicated. PD0332991, as a cyclin-dependent kinase inhibitor, can alter cell cycle control mechanisms, affecting the temporal expression or activity of ARMC12.

MLN4924's action on the NEDD8-activating enzyme can disrupt protein ubiquitination and stability, potentially influencing ARMC12-associated protein complexes. Inhibitors like GSK3β Inhibitor VIII and IWP-2 take aim at the Wnt signaling cascade, a fundamental pathway for cell fate determination and tissue patterning, where ARMC12 may have a role. Bortezomib and MG132 serve as proteasome inhibitors, which can lead to the accumulation of proteins and interfere with degradation pathways that might include ARMC12. Trichostatin A's inhibition of histone deacetylases can result in epigenetic changes, possibly affecting ARMC12 gene expression. Blocking γ-secretase with DAPT may influence Notch signaling, which is critical for cell communication and can intersect with ARMC12's function. SB431542 and LDN-193189 target TGF-β and BMP signaling, respectively; these pathways are instrumental in regulating cell growth and differentiation, potentially interacting with ARMC12. Lastly, Rapamycin's inhibition of mTOR signaling can result in broad effects on cell growth and autophagy, processes that may involve ARMC12.

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