Date published: 2025-10-29

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SCARA3 Inhibitors

SCARA3, also known as scavenger receptor class A member 3, is a transmembrane protein involved in various cellular processes, including phagocytosis, cell adhesion, and intracellular signaling. Functionally, SCARA3 plays a crucial role in innate immunity and cellular homeostasis by mediating the recognition and clearance of extracellular ligands, pathogens, and apoptotic cells. Structurally, SCARA3 contains a conserved scavenger receptor domain responsible for ligand binding and internalization. Additionally, SCARA3 interacts with intracellular signaling molecules to transduce extracellular signals and modulate cellular responses. Through its involvement in these processes, SCARA3 contributes to immune surveillance, inflammation regulation, and tissue homeostasis.

Inhibiting SCARA3 function involves targeting its associated signaling pathways and disrupting its interaction with intracellular effectors. Various chemicals have been identified as direct inhibitors of SCARA3-mediated signaling, primarily by targeting key signaling molecules involved in its activation and downstream signaling cascades. For instance, inhibition of the PI3K/Akt/mTOR pathway using compounds like Wortmannin and Rapamycin suppresses SCARA3 function by impeding its activation and downstream signaling. Similarly, inhibitors targeting MAPK pathways, such as PD98059 and U0126, disrupt SCARA3-mediated signaling by inhibiting its expression and downstream signaling events. Moreover, inhibition of NF-κB, JAK/STAT, and STAT3 pathways using specific inhibitors like BAY 11-7082, AG-490, and Cucurbitacin I, respectively, leads to down-regulation of SCARA3 expression and activity. Overall, targeting these signaling pathways represents a promising approach for inhibiting SCARA3 function and modulating its role in cellular immunity and homeostasis.

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