Date published: 2025-9-15

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granzyme C Inhibitors

Granzyme C inhibitors encompass a group of chemical compounds that can indirectly interfere with the enzymatic activity of granzyme C, a serine protease. These inhibitors primarily target the active site of serine proteases, where they can bind covalently or non-covalently to disrupt the normal function of the enzyme. The active site typically contains a serine residue that plays a critical role in the catalytic mechanism of the protease. Compounds such as AEBSF, PMSF, and 3,4-DCI are known to form irreversible bonds with the serine residue, thereby preventing substrate binding and subsequent proteolytic activity. Other inhibitors operate through reversible mechanisms. For example, Benzamidine Hydrochloride and Leupeptin Hemisulfate act as competitive inhibitors by mimicking the natural substrate of serine proteases. Aprotinin and Soybean Trypsin Inhibitor are protein-based inhibitors that block the active sites of serine proteases like granzyme C through complex formation. These inhibitors are not specific to granzyme C but can reduce its activity due to the shared characteristics of serine proteases' active sites.

The effectiveness of these inhibitors in reducing granzyme C activity is contingent upon their ability to access the active site and their affinity for the enzyme. Small synthetic molecules such as Gabexate Mesilate, Camostat Mesilate, and Nafamostat Mesilate have been designed to inhibit proteases and may interact with granzyme C similarly. Even though some inhibitors like Pepstatin A and E-64 are primarily targeted against other classes of proteases, they may exhibit off-target effects that include the inhibition of serine proteases. The utility of this class of inhibitors lies in their capacity to modulate the activity of granzyme C indirectly. By targeting the enzymatic function, these inhibitors can provide insights into the role of granzyme C in cellular processes. The broad specificityof these compounds requires careful consideration when interpreting their effects on granzyme C, as they can also affect other serine proteases with similar active sites. The chemical diversity of granzyme C inhibitors spans synthetic compounds, natural protein inhibitors, and peptide-like molecules, each with a unique mechanism of action but a common goal of modulating protease activity.

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