Date published: 2025-9-15

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KIF1A Inhibitors

KIF1A inhibitors encompass a range of chemicals that indirectly target the KIF1A protein by influencing related motor proteins and pathways involved in microtubule dynamics and cell division processes. While direct inhibitors of KIF1A are currently limited, these compounds offer a pathway to modulate KIF1A activity indirectly. The inhibitors primarily target kinesin-like proteins such as Eg5 and KSP, which share functional similarities with KIF1A, particularly in their roles in microtubule-based transport. These inhibitors function by disrupting the ATPase activity of target proteins, altering their binding to microtubules, or interfering with the spindle assembly processes. For example, compounds like Monastrol and Dimethylenastron act by specifically inhibiting Eg5, leading to changes in spindle dynamics that can indirectly impact KIF1A's role in vesicle transport and cell division. Similarly, Ispinesib and Filanesib target KSP, affecting microtubule stability and thereby potentially influencing KIF1A functions. The inhibition of these related proteins can lead to altered cellular transport mechanisms, affecting the transport of synaptic vesicles and other cargoes within neurons, where KIF1A plays a crucial role. Some inhibitors like ON 01910.Na and BI-2536 target kinases such as Plk1, which are involved in mitotic spindle formation. By interfering with these kinases, these inhibitors can indirectly modulate KIF1A's role in synaptic vesicle transport. The inhibition of Aurora kinases by compounds like ZM447439 and VX-680 also contributes to this indirect modulation, as these kinases are critical for spindle assembly and chromosome segregation during cell division.

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