Date published: 2025-9-18

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CDH20 Inhibitors

In describing CDH20 Inhibitors, these are chemicals that can affect the function of CDH20 indirectly by modulating calcium levels, influencing cell adhesion pathways, or altering the signaling context in which CDH20 operates. For instance, calcium chelators like EGTA and BAPTA-AM can sequester calcium ions necessary for the proper function of cadherins, including CDH20, thereby affecting their adhesion properties. The perturbation of calcium signaling can lead to changes in the conformation and adhesive functions of CDH20.

Other compounds, such as IWP-2 and XAV-939, target the Wnt signaling pathway, which is intimately connected with cadherin function. By modulating Wnt signaling, these inhibitors can indirectly influence the cellular behaviors that depend on cadherin-mediated adhesion. Inhibitors of the TGF-β pathway, like SB431542, can also impact cadherin function since TGF-β signaling is known to regulate cell adhesion and differentiation. Furthermore, compounds targeting the PI3K/Akt pathway and MAPK/ERK pathway have the capacity to influence cell adhesion dynamics and could thereby affect CDH20-mediated interactions. Additionally, the regulation of cadherin function can be influenced by agents that affect the Notch signaling pathway, such as DAPT, which inhibits gamma-secretase activity and can alter cell fate decisions that hinge on cell adhesion status. Inhibitors of GSK-3 can activate pathways like Wnt and thereby have consequences on cadherin-mediated processes. Blebbistatin, by inhibiting myosin II, can affect the cytoskeletal dynamics and force generation that are important for the maintenance of cell shape and tissue integrity where CDH20 plays a role.

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