Date published: 2025-9-13

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DDX24 Inhibitors

DDX24 inhibitors encompass a diverse set of chemicals that interfere with various cellular processes and signaling pathways, indirectly modulating the activity and function of the DEAD-box protein DDX24. These inhibitors do not directly target the DDX24 protein; instead, they impact the cellular environment, pathways, and processes that DDX24 is involved in or reliant upon. These chemicals can influence the stability, localization, post-translational modification, or expression of DDX24, thereby inhibiting its function.

The inhibitors range from compounds that affect the cell's genetic material, such as DNA replication and repair inhibitors, to those that disrupt cytoskeletal dynamics and protein stability. For example, paclitaxel and etoposide target key components of cell division and DNA processing affecting DDX24's role in these pathways. MG132 and 17-AAG focus on protein degradation systems, which could lead to DDX24 accumulation or degradation, respectively. Compounds like LY294002 and wortmannin act on PI3K, altering cell survival pathways that can indirectly affect DDX24's function. Staurosporine's broad kinase inhibition could modify the phosphorylation status of DDX24, impacting its activity. In contrast, 5-azacytidine and actinomycin D modify gene expression patterns and transcription processes, altering DDX24 expression levels. Chloroquine, by altering endosomal and lysosomal function, can impact the cellular localization and degradation pathways of DDX24. Each chemical in this class acts through unique mechanisms, but all converge on the common outcome of modulating DDX24's function. The diverse mechanisms ofaction reflect the complex regulation of DDX24 and the intricate cellular networks in which it operates. These inhibitors offer valuable tools for dissecting the role of DDX24 in cellular processes and elucidating the biochemical pathways it influences.

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