Date published: 2025-9-18

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SLC17A4 Activators

SLC17A4 activators are distinct chemical entities that are specifically designed to intensify the functional performance of SLC17A4, a protein that plays a pivotal role in the transport of uridine monophosphate. These activators operate through several direct and indirect pathways, each lending a unique and critical influence on the protein's activity. The direct enhancement of SLC17A4's functionality occurs through the provision of ATP. As a coenzyme, ATP provides the necessary energy for the protein's transport function, making it an integral part of SLC17A4's activity. Uridine, another direct activator, is a nucleoside that forms a component of uridine monophosphate. An increase in the pool of uridine leads to an increased substrate for SLC17A4 to transport, thus indirectly enhancing its functionality.

On the other hand, indirect activators including Glucose, Fructose, Adenosine, Sodium Chloride, Insulin, Creatine, Pyruvate, Citrate, Lactate, and Aspartate operate through a range of cellular processes that eventually lead to the provision of ATP. By influencing these processes, these activators indirectly contribute to enhancing SLC17A4's activity. Glucose, Fructose, and Adenosine, for example, undergo metabolic processes that lead to the generation of ATP, which is then used to power the transport function of SLC17A4. Sodium Chloride, on the other hand, plays a key role in maintaining the electrochemical gradient across the membrane, a factor that significantly affects the transport function of SLC17A4. Insulin regulates glucose metabolism, which indirectly affects ATP production and, in turn, the activity of SLC17A4. The roles of Creatine, Pyruvate, Citrate, Lactate, and Aspartate are tied to their contributions to the metabolic processes that generate ATP.

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