Date published: 2025-11-7

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OTTMUSG00000010130 Inhibitors

The selected chemicals target a range of cellular processes and pathways that could potentially affect the function of the pramel family member protein. Inhibitors like Cycloheximide and Rapamycin affect protein synthesis and mTOR signaling, respectively, which might impact the synthesis or functional environment of the pramel family member protein. Staurosporine's broad kinase inhibition might affect kinase-dependent pathways potentially relevant to the function of this protein. Bortezomib's proteasome inhibition could influence the pramel family member protein by impacting protein degradation mechanisms, potentially affecting its turnover or function. Chloroquine's disruption of lysosomal function and autophagy could also indirectly affect the pramel family member protein by altering the degradation or processing of proteins. Wortmannin and LY294002, as PI3K inhibitors, might influence the protein by impacting PI3K/Akt signaling pathways, crucial for various cellular processes.

U0126 and PD98059, targeting MEK in the MAPK/ERK pathway, might modulate cell signaling and proliferation pathways, possibly influencing the pramel family member protein's activity. Curcumin's anti-inflammatory effects might modulate cellular signaling pathways, potentially impacting the protein's function if it is involved in related stress or inflammatory responses. SB203580 and Z-VAD-FMK target the p38 MAPK and apoptotic pathways, respectively, and could potentially affect the pramel family member protein through these complex signaling networks. These inhibitors, through their actions on various cellular mechanisms, may indirectly influence the activity and function of the pramel family member protein. This approach is broad and non-specific due to the lack of direct inhibitors and is based on the potential involvement of this protein in various cellular pathways. The selection illustrates the interconnected nature of cellular signaling and the challenges in targeting specific proteins without direct inhibitors.

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