Date published: 2025-10-12

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CCDC75 Inhibitors

Roscovitine, Paclitaxel, and Nocodazole are agents that modulate cell cycle progression and mitotic spindle function. Through their action on these fundamental cellular mechanisms, they can impact proteins associated with cell division, which may include CCDC75. Lithium Chloride, U0126, LY294002, SB431542, and Rapamycin are inhibitors that target critical signaling pathways, such as GSK-3, MEK/ERK, PI3K/AKT, TGF-β, and mTOR pathways, respectively. These pathways are central to processes such as transcriptional regulation, protein synthesis, and autophagy. Inhibiting these pathways can influence the levels and activity of a range of proteins, CCDC75 being one of them, if it is part of or regulated by these pathways.

Trichostatin A and MG132 affect epigenetic regulation and protein degradation. Trichostatin A changes the chromatin landscape, potentially altering gene expression profiles, while MG132 prevents the degradation of proteins, which can lead to an accumulation of a wide array of cellular proteins, including CCDC75 if it is subject to proteasomal degradation. Y-27632, by inhibiting ROCK, can affect the organization of the cytoskeleton, and Bafilomycin A1, by inhibiting V-ATPase, can disrupt the acidification of endosomes and lysosomes, processes that may be critical for the cellular localization and degradation of CCDC75.

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