Date published: 2025-11-28

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Morc Inhibitors

Chemical inhibitors of Morc can function through a variety of mechanisms that alter the chromatin landscape, which is central to Morc's role in the cell. Trichostatin A, Nicotinamide, SAHA (Vorinostat), RGFP966, and Scriptaid are all inhibitors of histone deacetylases (HDACs). These inhibitors can increase the acetylation levels of histones, leading to a more open chromatin conformation and, consequently, affecting the ability of Morc to bind and modify chromatin. For instance, Trichostatin A and SAHA can induce hyperacetylation of histones, which may prevent Morc from accessing its usual binding sites or from exerting its chromatin remodeling functions. Similarly, RGFP966's selective inhibition of HDAC3 and Scriptaid's inhibition of HDACs can disrupt Morc's interaction with chromatin by altering the histone acetylation pattern, which is a crucial determinant of Morc's functional engagement with chromatin.

Additionally, chemicals like Chloroquine and Mithramycin A can directly bind to DNA, impacting Morc's ability to interact with and modify chromatin. Chloroquine intercalates into DNA, which can inhibit DNA and RNA synthesis, effectively altering the chromatin state and impeding Morc's function. Mithramycin A, by binding to DNA, can prevent Morc from accessing its chromatin targets. Similarly, Distamycin and Echinomycin act by binding to DNA structures; Distamycin binds to the minor groove, and Echinomycin acts as a bis-intercalator. Both of these can obstruct the DNA binding sites that Morc may require for its chromatin remodeling activities. Camptothecin, a topoisomerase I inhibitor, can induce DNA damage and alter DNA accessibility, which in turn can affect Morc's role in chromatin remodeling by modifying the DNA structure with which Morc interacts. Lastly, Caffeine affects various signaling pathways and influences chromatin remodeling processes, which can alter Morc's chromatin interactions and inhibit its function in the cell. By targeting different aspects of chromatin structure and function, these chemical inhibitors can compromise the ability of Morc to fulfill its role in chromatin remodeling.

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