Date published: 2025-9-15

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TCP-1 ε Activators

TCP-1 ε activators are a class of chemicals that directly or indirectly enhance the functional activity of TCP-1 ε, a molecular chaperone involved in the folding of proteins upon ATP hydrolysis. This class includes chemicals that act by various mechanisms, including those that enhance ATPase activity, interfere with phosphorylation states, stabilize protein structures, and mediate cellular stress responses. For example, Ascorbic acid acts as a reducing agent, restoring the native conformation of TCP-1 ε and enhancing its chaperone function. ATP, as the direct energy source for TCP-1 ε's protein folding function, can enhance its ATPase activity, promoting the protein folding process. Zinc sulfate and Calcium chloride stabilize protein structures, enhancing the chaperone function of TCP-1 ε indirectly.

On the other hand, Sodium orthovanadate, Forskolin, Phorbol 12-myristate 13-acetate (PMA), Okadaic acid, and Lithium chloride influence the phosphorylation state of TCP-1 ε, potentially enhancing its function. Sodium orthovanadate inhibits protein tyrosine phosphatases, influencing the phosphorylation state of TCP-1 ε and possibly enhancing its chaperone function. Forskolin, an activator of protein kinase A (PKA), and PMA, an activator of protein kinase C (PKC), can lead to the phosphorylation of TCP-1 ε, potentially enhancing its function. Okadaic acid and Lithium chloride inhibit protein phosphatases and GSK3β respectively, preventing the dephosphorylation of TCP-1 ε and possibly enhancing its function. Lastly, Sodium arsenite and Phosphatidylserine enhance TCP-1 ε function by inducing cellular stress responses and binding to TCP-1 ε respectively. These chemicals collectively provide a range of ways to enhance the functional activity of TCP-1 ε, thereby helping to maintain the balance of protein homeostasis

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