Date published: 2025-10-12

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HEATR2 Inhibitors

The chemical class of HEATR2 inhibitors, as outlined here, focuses on compounds that indirectly target the function and regulation of HEATR2, primarily through pathways associated with ciliary function and assembly. Since HEATR2 is integral to ciliary dynamics, influencing pathways like Wnt signaling, mTOR signaling, and actin filament organization provides a strategy to modulate its activity. Lithium chloride, for example, modulates Wnt signaling, a key pathway in ciliogenesis. By altering this pathway, it may impact the assembly and function of cilia where HEATR2 plays a role. Similarly, compounds like roscovitine and rapamycin, which target cyclin-dependent kinases and mTOR respectively, offer an indirect approach to influence ciliary dynamics. These compounds, by modifying cell cycle regulation and cellular growth pathways, could affect the structure and function of cilia, thereby modulating HEATR2's activity.

Other compounds in this class, such as forskolin and cytochalasin D, act by altering intracellular signaling mechanisms and cytoskeletal dynamics. Forskolin increases cAMP levels, which are known to regulate ciliary beat frequency and could thus affect HEATR2's role in ciliary motility. Cytochalasin D, on the other hand, disrupts actin filaments, which are crucial for the structural integrity and function of cilia. Moreover, agents like chlorpromazine and bafilomycin A1, which influence ciliary membrane composition and protein trafficking, respectively, highlight the complexity of targeting HEATR2 activity. The diversity of these mechanisms underlines the multifaceted approach required to modulate ciliary function and, by extension, HEATR2 activity. In summary, the chemical class of HEATR2 inhibitors comprises compounds that indirectly influence HEATR2 by targeting various pathways and processes critical to ciliary assembly, function, and maintenance. This approach is pivotal in understanding and potentially modulating the role of HEATR2, especially in the context of diseases like primary ciliary dyskinesia, where ciliary dysfunction is a key feature.

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