Date published: 2025-12-16

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FASP1 Activators

The category of FASP1 Activators represents a group of chemicals known for their potential to indirectly influence the activation of FASP1 (MIS18A), a protein involved in chromatin assembly and related cellular processes. These activators exert their effects through various mechanisms, primarily targeting key cellular pathways that indirectly impact FASP1 activation. Chemicals within this class include compounds like Trichostatin A, Etoposide, Nocodazole, Puromycin, Hydroxyurea, Valproic Acid, Paclitaxel, Vorinostat, Aphidicolin, Actinomycin D, Camptothecin, and Bleomycin. Trichostatin A and Vorinostat are histone deacetylase inhibitors that modify histone acetylation patterns, potentially altering chromatin structure and indirectly activating FASP1. Etoposide, by inhibiting topoisomerase II, impacts DNA integrity, leading to changes in chromatin organization that can indirectly influence FASP1 activation.

Nocodazole disrupts microtubule dynamics, critical for proper chromosome segregation during cell division, indirectly affecting chromatin assembly processes and potentially activating FASP1. Puromycin interferes with protein synthesis, potentially reducing the availability of chromatin assembly factors and indirectly promoting FASP1 activation. Hydroxyurea inhibits ribonucleotide reductase, essential for DNA synthesis, thereby indirectly influencing chromatin assembly and FASP1 activation. Valproic Acid and Vorinostat, both histone deacetylase inhibitors, modify histone acetylation patterns, potentially affecting chromatin structure and indirectly promoting FASP1 activation. Paclitaxel stabilizes microtubules, affecting mitotic spindle formation and chromatin dynamics, indirectly influencing FASP1 activation. Aphidicolin inhibits DNA polymerases, potentially altering DNA replication dynamics and indirectly promoting FASP1 activation. Actinomycin D inhibits transcription by RNA polymerase, leading to changes in gene expression patterns that can indirectly influence various cellular processes, including chromatin assembly, and promote FASP1 activation. Camptothecin, a topoisomerase I inhibitor, impacts DNA topology, indirectly altering chromatin organization and promoting FASP1 activation. Bleomycin is a DNA-damaging agent that disrupts DNA integrity, potentially leading to changes in DNA structure and chromatin-related processes, ultimately promoting FASP1 activation.

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