Date published: 2025-9-15

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TMEM118 Activators

The chemical class termed as TMEM118 activators primarily converges around the modulation of cyclic nucleotide levels in the cell, especially cAMP and cGMP. These cyclic nucleotides serve as crucial secondary messengers in numerous intracellular signaling pathways. Through chemicals like Forskolin, which directly activate adenylyl cyclase, or via the inhibition of PDEs (phosphodiesterases) by agents like Rolipram or Exisulind, the intracellular concentration of cAMP or cGMP can be heightened. Elevated cAMP, for instance, activates Protein Kinase A (PKA), leading to a cascade of intracellular events.

The intricacies of TMEM118's function may intertwine with these cascades, making it plausible to modulate the protein indirectly by targeting cyclic nucleotide concentrations. Another approach involves the use of chemicals like PGE2 or NECA, which function by directly or indirectly stimulating the adenylate cyclase enzyme. This enzyme plays a pivotal role in cAMP synthesis, thereby influencing all downstream cAMP-mediated events. Similarly, chemicals that inhibit specific PDE isoforms cater to the same objective but through a different mechanism. Vinpocetine, for instance, specifically inhibits PDE1, leading to elevated cGMP levels. This elevation can modulate certain cellular pathways which TMEM118 may be a part of. Essentially, the modulation of cyclic nucleotide concentrations forms the crux of the proposed chemical activation strategy. By carefully selecting agents that either elevate these nucleotides or sustain their high levels, cellular processes can be influenced in ways that may impact the function or expression of TMEM118. These chemicals, despite not being direct activators of TMEM118, provide an indirect approach to influence the protein. The overarching theme among them is their ability to modulate intracellular signaling by primarily targeting cyclic nucleotide levels, offering a method to influence the protein TMEM118 and its associated cellular functions.

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