CIDE-C Activators encompass a range of chemical compounds that indirectly stimulate CIDE-C's functional role in lipid metabolism and energy homeostasis. Forskolin and IBMX, through the elevation of intracellular cAMP levels, activate protein kinase A (PKA), which in turn may enhance the lipolytic function of CIDE-C by promoting the breakdown of lipid droplets. Similarly, the availability of substrates such as palmitic and oleic acids can be conducive to the lipid droplet association and activity of CIDE-C, possibly facilitating the mobilization of stored fats. The metabolic modulators like rosiglitazone and pioglitazone exert their effects via PPARγ agonism, which can lead to an upregulated metabolic gene expression profile that includes pathways where CIDE-C is actively involved, thereby enhancing its functional role without directly influencing its expression levels.
Furthermore, compounds such as NAD+ and L-Carnitine influence CIDE-C activity by modifying its post-translational state and fatty acid flux, respectively. NAD+ serves as a substrate for sirtuins that may activate CIDE-C by deacetylation, whereas L-Carnitine is essential for fatty acid transport into mitochondria for β-oxidation, thereby increasing the substrate turnover for CIDE-C. Retinoic acid and GW 7647, through their roles as ligands for nuclear receptors, can shift theexpression of metabolic genes, creating a favorable environment for CIDE-C's involvement in lipid handling. The array of activators also includes choline, which by contributing to phospholipid synthesis, may support cellular membrane dynamics and lipid signaling, processes that are integral to the functional enhancement of CIDE-C. Epinephrine's role as an activator is also noteworthy; it binds to beta-adrenergic receptors, triggering a cascade that culminates in the activation of PKA, which can promote CIDE-C's activity by stimulating lipolysis and lipid mobilization. This mechanism is key to the body's response to energy demands, and epinephrine ensures that CIDE-C is functionally ready to orchestrate the rapid release of fatty acids when necessary. Collectively, these activators operate through distinct yet interconnected pathways, converging on the facilitation of CIDE-C's role in managing lipid distribution and utilization within cells, thus highlighting the multifaceted regulation of this protein's activity in energy homeostasis.
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