Date published: 2025-9-20

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Gm216 Inhibitors

The chemical class termed Catip Inhibitors refers to a variety of compounds that can indirectly modulate the activity of Catip by influencing ciliogenesis and its associated pathways. These compounds employ diverse mechanisms to interfere with the processes and structures crucial for the proper formation and function of cilia, where Catip is thought to play a role. Cytochalasin D and Latrunculin A, for example, hinder actin polymerization, a necessary step in ciliogenesis, thereby potentially limiting Catip's function. Similarly, Colchicine's ability to prevent tubulin polymerization can impede the formation of cilia, indirectly affecting Catip activity.

On the other hand, compounds like Forskolin and Genistein modulate signaling pathways that are critical for ciliogenesis. Forskolin elevates intracellular cAMP levels, which are known to play a role in the regulation of ciliogenesis, while Genistein inhibits tyrosine kinases that can signal for ciliogenesis. Rapamycin, an mTOR inhibitor, and PF-670462, a casein kinase 1 inhibitor, can disrupt the signaling pathways that regulate cilia length and function, potentially altering Catip's involvement in these processes. Bepridil, which affects calcium channels, can also modulate calcium-dependent ciliogenesis processes, thereby possibly influencing Catip. Furthermore, compounds like Chlorpromazine and Nitrofurantoin, although not specifically targeting ciliogenesis, can affect cellular signaling and membrane dynamics, potentially exerting an indirect effect on Catip. Y-27632, by inhibiting Rho-associated protein kinase (ROCK), can alter cytoskeletal organization, which is a prerequisite for ciliogenesis and thus may impact Catip's function. Lastly, Oxindole, with its protein kinase inhibition properties, could affect the broader signaling pathways involved in ciliogenesis, hence potentially affecting Catip's role in the process.

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