Date published: 2025-9-17

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ZPBP1 Inhibitors

Chemical inhibitors of Zona Pellucida Binding Protein 1 (ZPBP1) can effectively hinder its function through various biochemical pathways. Phloretin, a compound known for its ability to impede glucose transporters, can interfere with the glycosylation process essential for the proper functioning of ZPBP1. A lack of glycosylation substrates due to the action of phloretin can lead to a functional impairment of ZPBP1. Similarly, Genistein targets tyrosine kinases, enzymes responsible for the phosphorylation of many proteins, including ZPBP1. By inhibiting these kinases, Genistein can reduce the phosphorylation crucial for ZPBP1 activity, leading to its inhibition. Another kinase inhibitor, PD 98059, obstructs MEK activity, which is pivotal for the phosphorylation processes within cells. This inhibition can prevent essential phosphorylation of ZPBP1, thereby impeding its functional activity.

Furthermore, LY294002 and Wortmannin, both inhibitors of PI3K, can thwart signaling pathways that are essential for ZPBP1's role in the cell. The inhibition of PI3K by these chemicals can lead to downstream effects that impede ZPBP1's involvement in crucial signaling cascades. SB203580 and SP600125, as inhibitors of p38 MAPK and JNK respectively, can disrupt the cellular stress response pathways where ZPBP1 may play a role, thus indirectly inhibiting its function. Gö 6983 and Bisindolylmaleimide I, both inhibitors of PKC, can prevent the phosphorylation of ZPBP1, thereby impeding its activity related to cell signaling and regulation. Y-27632, a ROCK inhibitor, can disrupt the dynamics of the actin cytoskeleton, possibly leading to an indirect functional inhibition of ZPBP1, which is implicated in maintaining cell structure. Lastly, BAPTA-AM, by chelating intracellular calcium, can disrupt ZPBP1-related calcium-dependent processes, further contributing to the inhibition of ZPBP1's function within the cell.

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