Date published: 2025-9-16

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DDX54 Inhibitors

DDX54 inhibitors are a class of chemicals that indirectly affect the function of the DDX54 protein through various mechanisms that impact cellular processes and pathways with which DDX54 is associated. These chemicals can alter DNA replication, transcription, protein synthesis, nuclear-cytoplasmic transport, and protein stability, all of which may influence the activity of DDX54.

The molecular actions of these inhibitors range from disruption of DNA replication and repair, where DDX54 is postulated to participate, to interference with RNA synthesis, which can affect the expression levels of DDX54. Compounds like Aphidicolin inhibit DNA polymerases, potentially limiting the availability of DNA templates that DDX54 acts upon. Actinomycin D and Homoharringtonine disrupt RNA and protein synthesis pathways, respectively, leading to reduced expression or availability of DDX54. Nuclear export inhibitors like Leptomycin B can prevent the proper localization of DDX54, impairing its function. Microtubule-stabilizing agents like Paclitaxel can indirectly affect DDX54 by disrupting cellular division, while proteasome and lysosome pathway inhibitors, such as MG132 and Chloroquine, respectively, can impact the degradation and turnover of DDX54. Lastly, topoisomerase inhibitors such as Camptothecin, Etoposide, and SN-38 can induce DNA damage and may influence the DNA repair functions in which DDX54 is speculated to be involved. These inhibitors do not share a common chemical structure or target but are linked by their ability to modulate the cellular environment and processes that govern the function of DDX54. The inhibition exerted by these compounds underscores the multifaceted roles that DDX54 may play in cellular physiology and the complex interplay between different biomolecular pathways.

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