Date published: 2025-10-12

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PCDHA4 Inhibitors

Chemical inhibitors classified as PCDHA4 inhibitors are compounds that indirectly modulate the function of PCDHA4 by influencing cell adhesion and signaling pathways rather than directly binding to or modifying the protein itself. PCDHA4 is a member of the cadherin family, which is known to mediate cellular adhesion through calcium-dependent interactions. The adhesion function of PCDHA4 is integral to its role in maintaining cell-cell contacts and signaling within the cellular environment.

Calcium chelators like EGTA can disrupt the calcium-dependent adhesion mechanism of PCDHA4, leading to a loss of cell-cell adhesion. Inhibitors of kinases such as Rho-associated protein kinase (Y-27632), Src family kinases (PP2), and mitogen-activated protein kinases (SB203580, SP600125, PD98059) can impact the signaling cascades that regulate cellular dynamics and interactions, which in turn can modulate the function of PCDHA4 in maintaining cellular cohesion. Additionally, the inhibition of phosphoinositide 3-kinases (Wortmannin) can perturb cell migration and adhesion, processes in which PCDHA4 is likely involved. Compounds like GM6001 prevent the remodeling of the extracellular matrix by inhibiting matrix metalloproteinases, which indirectly affects the context in which PCDHA4 operates. Similarly, XAV-939 and SB-216763 interfere with Wnt/β-catenin and GSK-3β signaling pathways, respectively, which are crucial for the regulation of cadherin-catenin complexes and may thus influence the functional dynamics of PCDHA4. By antagonizing N-cadherin (ADH-1), the balance of adhesion forces may be shifted, indirectly impacting PCDHA4's role in the adhesion network. Geldanamycin's binding to HSP90 can also modify the stability and function of proteins involved in signaling pathways, potentially affecting PCDHA4-related processes.

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