The chemical class SMC1β Activators encompasses a range of compounds that might indirectly modulate the activity of SMC1β, a key protein in chromosome cohesion and segregation during meiosis. These compounds do not interact directly with SMC1β but potentially influence cellular pathways and mechanisms integral to chromosomal dynamics and DNA repair, wherein SMC1β plays a crucial role. DNA damage-inducing agents, such as Camptothecin and Etoposide, which inhibit topoisomerase enzymes, and Mitomycin C, which induces DNA crosslinking, are significant representatives of this class. By inducing DNA damage, these compounds could trigger cellular DNA repair mechanisms, potentially influencing the activity of SMC1β in response to altered chromosomal dynamics. Similarly, Hydroxyurea and Aphidicolin, affecting DNA synthesis and replication, could indirectly impact SMC1β activity by modulating the cellular environment during meiosis, a critical process involving SMC1β.
Additionally, Caffeine and Bleomycin, known for their effects on DNA repair pathways and cellular stress responses, might also indirectly affect SMC1β. This indirect influence underscores the complex interplay between DNA damage response and chromosomal regulation in which SMC1β is involved. Furthermore, compounds like Olaparib, a PARP inhibitor, and Gemcitabine, a nucleoside analog, could influence SMC1β activity by affecting homologous recombination and DNA replication processes, respectively.
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