Date published: 2025-12-15

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ASNSD1 Activators

Forskolin, IBMX, and Dibutyryl-cAMP share a commonality in their approach to ASNSD1 activation through the elevation of intracellular cAMP levels. This increase in cAMP activates PKA, which phosphorylates numerous proteins, potentially influencing the activity of ASNSD1. Zinc sulfate enters the cellular framework with a different role, possibly serving as a critical cofactor that ensures proper structural conformation and enzymatic function of ASNSD1. Another aspect of this intricate regulatory network involves the preservation of phosphorylation states, a role adeptly played by sodium orthovanadate. By inhibiting protein tyrosine phosphatases, this compound maintains proteins in a phosphorylated state, which may be crucial for the active conformation of ASNSD1. PMA, through its activation of PKC, introduces another layer of control, modulating protein phosphorylation and thereby influencing ASNSD1's activity.

Resveratrol emerges as a modulator of protein acetylation via the activation of sirtuins. This modulation of acetylation states can have profound effects on protein interactions and functions, possibly impacting the regulation of ASNSD1. Moreover, kinase inhibitors such as LY294002, U0126, SB203580, and SP600125 each play a role in adjusting the phosphorylation landscape within the cell. By targeting specific kinases like PI3K, MEK, p38 MAPK, and JNK, these inhibitors can shift the balance of kinase and phosphatase activities, which in turn can affect the proteins that regulate ASNSD1.

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