Date published: 2025-9-5

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NMT1 Activators

NMT1 Activators, in the context of indirect enhancement of NMT1's enzymatic activity, encompass a range of compounds primarily influencing lipid metabolism and availability within cells. Myristic Acid, being the direct substrate for NMT1, stands out as a key factor; an increase in its intracellular concentration could enhance NMT1's activity by providing more substrate for the myristoylation process. Similarly, Palmitic Acid, though not a direct substrate, can influence lipid metabolism pathways, potentially altering fatty acid availability and distribution, which might indirectly impact NMT1 activity. Compounds like Forskolin, which increases intracellular cAMP and activates PKA, could also influence NMT1 activity indirectly by phosphorylating proteins involved in lipid metabolism. In addition to these, lipids such as D-erythro-Sphingosine might create a cellular environment conducive to enhanced NMT1 activity by influencing cellular lipid distribution and metabolism.

Agents like LY 294002, a PI3K inhibitor, and U-73122, a PLC inhibitor, modulate cellular signaling pathways related to growth and lipid metabolism, potentially impacting NMT1 indirectly. The mTOR inhibitor Rapamycin and AMPK activators such as AICAR and Metformin play roles in regulating cellular energy balance and lipid metabolism, which could indirectly affect NMT1's activity by altering the availability of fatty acids. Furthermore, Pioglitazone, a PPAR-gamma agonist, and Lovastatin, an HMG-CoA reductase inhibitor, both influence lipid metabolism in ways that could potentially impact NMT1 activity. Elevated levels of Cholesterol, a key component of cellular membranes, could also indirectly influence NMT1 activity by altering the balance of fatty acids available for the myristoylation process. Collectively, these compounds, through their effects on cellular lipid metabolism and distribution, illustrate the complex regulation of NMT1 activity, a critical enzyme in post-translational modification and cellular signaling.

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