Date published: 2025-9-16

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DHRS4 Activators

DHRS4 activators include a diverse array of compounds that, through their interaction with various cellular pathways, indirectly support the upregulation and enhancement of DHRS4 activity. For instance, some of these activators work by increasing intracellular cyclic AMP (cAMP) levels, which is achieved through either direct stimulation of adenylate cyclase or inhibition of phosphodiesterase enzymes. The elevated cAMP levels can lead to enhanced protein phosphorylation processes, potentially increasing DHRS4 activity. Another subset of activators impacts the cellular energy balance by activating AMP-activated protein kinase (AMPK), which in turn, may lead to the upregulation of DHRS4 activity by modulating metabolic pathways that are sensitive to the energy status of the cell. Moreover, certain activators can influence the cellular redox state, which is closely linked to DHRS4 function, by altering the NAD+/NADH ratio or by modulating the activity of Nrf2, a key regulator of the oxidative stress response.

Further, compounds that modulate specific signaling molecules or pathways, such as protein kinase C (PKC), PPAR-gamma, or NF-kB, also play a role in the indirect activation of DHRS4. For example, PKC activation can lead to a cascade of phosphorylation events, which may include proteins that are part of DHRS4's functional pathway. PPAR-gamma agonists and NF-kB pathway modulators are known to influence gene expression and inflammatory responses, which could in turn affect DHRS4 activity in relation to lipid metabolism and redox balance. Additionally, sirtuin activators and GSK-3 inhibitors interact with signaling networks that are implicated in cellular metabolism and Wnt signaling, respectively, suggesting that these activators could also support the enhancement of DHRS4 activity by modulating metabolic processes or signaling pathways relevant to its function.

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