Date published: 2025-9-13

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PUS3 Inhibitors

PUS3 inhibitors are chemical compounds that specifically target and inhibit the function of the Pseudouridine Synthase 3 (PUS3) enzyme, a member of the pseudouridine synthase family. PUS3 is responsible for catalyzing the isomerization of uridine to pseudouridine, which is an essential post-transcriptional modification found in various types of RNA, including tRNA and mRNA. This modification enhances RNA stability and contributes to proper RNA folding and function. By inhibiting PUS3, these compounds disrupt the enzyme's catalytic activity, reducing or preventing the formation of pseudouridine in RNA. PUS3 inhibitors are of interest in biochemical research for their ability to modulate RNA structure and function, providing insight into the role of pseudouridylation in RNA biology. Additionally, by blocking PUS3 activity, these inhibitors can be valuable tools for investigating how changes in RNA modifications affect cellular processes, including translation efficiency, RNA-protein interactions, and cellular stress responses.

The structure of PUS3 inhibitors typically involves small molecules that can selectively bind to the active site of the enzyme, preventing its interaction with RNA substrates. These inhibitors may be designed to interact with key residues within the active site pocket or to alter the conformation of the enzyme, rendering it inactive. The specificity and efficacy of PUS3 inhibitors are highly dependent on their chemical structure, which is often optimized through medicinal chemistry techniques to enhance binding affinity and stability. Additionally, understanding the structural biology of PUS3 allows for a rational design approach, in which modifications to the chemical structure of these inhibitors can improve their potency and selectivity. Researchers are particularly interested in PUS3 inhibitors to explore the biological consequences of altered pseudouridylation, as well as to develop new methods for controlling RNA processing and function in various cellular contexts.

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