Date published: 2025-9-16

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PSD4 Inhibitors

PSD4 inhibitors are a class of chemical compounds that specifically target the Pleckstrin and Sec7 domain-containing protein 4 (PSD4), a guanine nucleotide exchange factor (GEF) involved in the regulation of intracellular signaling pathways. PSD4 belongs to the cytohesin family of GEFs, which are responsible for the activation of small GTPases, including ARF (ADP-ribosylation factor) proteins. By facilitating the exchange of GDP for GTP on ARF proteins, PSD4 plays a critical role in controlling cellular processes like membrane trafficking, cytoskeletal dynamics, and vesicular transport. Inhibitors of PSD4 act by binding to its active site or allosteric regions, thereby impeding its ability to catalyze the nucleotide exchange process. This inhibition can result in altered ARF signaling and downstream cellular effects, including changes in cell morphology, migration, and signal transduction. Because PSD4 is involved in critical cellular functions, its inhibition can significantly impact various intracellular pathways.

The structure of PSD4 inhibitors is often designed to target specific binding sites within the PSD4 protein, such as the Sec7 domain responsible for its GEF activity. These inhibitors vary in their chemical composition and binding affinity, but they generally possess structural features that allow for selective and high-affinity interactions with PSD4. Additionally, the development of PSD4 inhibitors requires careful consideration of their specificity, as the cytohesin family contains closely related proteins with similar domains and functions. The precise structure-activity relationships (SAR) of PSD4 inhibitors are critical for ensuring that they effectively target PSD4 without affecting other GEFs or ARF regulators. Moreover, the physicochemical properties of these inhibitors, such as their solubility, stability, and permeability, play a crucial role in their overall activity and bioavailability. Understanding these characteristics enables a deeper exploration of PSD4's biological role and its regulatory mechanisms in various cellular contexts.

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