ITPase inhibitors are a class of chemical compounds that specifically target and inhibit the activity of inosine triphosphate pyrophosphatase (ITPase), an enzyme responsible for hydrolyzing inosine triphosphate (ITP) to inosine monophosphate (IMP) and inorganic pyrophosphate. ITPase plays a critical role in maintaining the purity of the nucleotide pool within cells by preventing the accumulation of non-canonical nucleotides like ITP, xanthosine triphosphate (XTP), and deoxyinosine triphosphate (dITP). These non-standard nucleotides, if incorporated into RNA or DNA, can lead to errors in transcription and replication, potentially causing cellular dysfunction. Inhibiting ITPase disrupts its ability to hydrolyze these non-canonical nucleotides, resulting in altered nucleotide pool dynamics and providing a means to study how nucleotide imbalances affect cellular processes.
The design of ITPase inhibitors typically focuses on targeting the enzyme's active site, where the hydrolysis of ITP occurs. These inhibitors often mimic the structure of ITP or its analogs, competing for binding at the enzyme's active site and preventing its normal catalytic activity. The binding of ITPase inhibitors is mediated by non-covalent interactions, such as hydrogen bonding, ionic interactions, and van der Waals forces, ensuring specificity and stability of the inhibitor-enzyme complex. By inhibiting ITPase, researchers can explore how the enzyme regulates nucleotide homeostasis and the impact of non-canonical nucleotide accumulation on cellular metabolism, transcription, and replication fidelity. These inhibitors are valuable tools for understanding the fundamental role of ITPase in maintaining the integrity of nucleotide pools and preventing the incorporation of potentially harmful nucleotides into nucleic acids.
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