Date published: 2025-9-14

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DNAH7 Inhibitors

The chemical class known as DNAH7 Inhibitors encompasses a diverse range of compounds that can indirectly affect the function of Dynein Axonemal Heavy Chain 7, a ciliary motor protein. This group of inhibitors acts not by directly binding to DNAH7 but by modifying the cellular environment and structures that are crucial for its activity. Microtubule-targeting agents, such as nocodazole, vinblastine, and colchicine, are central to this category. These compounds can disrupt the polymerization of microtubules, the structural tracks along which DNAH7 moves. By destabilizing these tracks, these agents prevent the normal function of DNAH7 in ciliary movement. Similarly, taxol, a microtubule-stabilizing agent, can inhibit DNAH7 by overly stabilizing microtubules, thereby reducing the dynamic range necessary for DNAH7 function. On the other hand, cytoskeletal disruptors like cytochalasin D and dihydrocytochalasin B, primarily known for their action on actin filaments, can also indirectly affect DNAH7 activity by causing a cascade of changes in cellular transport mechanisms that rely on actin and microtubule interplay.

Further, compounds like ciliobrevin D and EHNA hydrochloride, which target dynein ATPase activity, can impede the energy-dependent mechanical actions of DNAH7, resulting in the inhibition of its motor functions. These inhibitors block the conversion of ATP to ADP and phosphate, which is the fundamental energy source for dynein motor proteins. Additionally, chemicals like brefeldin A and monastrol affect vesicle transport and kinesin motor activity, respectively, and these disruptions in cellular transport logistics can create a ripple effect that impacts the function of dynein motors, including DNAH7. Lithium, an element known for its influence on the GSK-3 enzyme and the Wnt signaling pathway, is implicated in the modulation of ciliogenesis. Alterations in these signaling pathways can lead to changes in ciliary structure and function, thereby indirectly affecting DNAH7.

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