Date published: 2025-10-12

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FOXO1 Activators

FOXO1, short for Forkhead box protein O1, is an intricately regulated transcription factor with a pivotal role in the orchestration of cellular responses to a variety of stimuli. It is a member of the O class of forkhead box transcription factors, recognized by a conserved winged-helix DNA-binding domain. FOXO1's involvement spans several cellular processes, including glucose metabolism, oxidative stress response, cell cycle regulation, and apoptosis. It is a substrate for several kinases, including AKT, SGK, and IKK, which regulate its activity through phosphorylation. This post-translational modification typically results in the sequestration of FOXO1 in the cytoplasm, inhibiting its transcriptional activity. Conversely, dephosphorylation of FOXO1 leads to its translocation into the nucleus, where it can activate the transcription of genes responsible for various cellular functions. The precise regulation of FOXO1 is thus critical to maintaining cellular homeostasis and responding to environmental changes.

A range of chemical compounds has been identified that can potentially induce the expression of FOXO1. These activators interact with cellular signaling pathways, often leading to changes in the phosphorylation status of FOXO1 and its subsequent activation. For instance, compounds like resveratrol and metformin are known to exert influence on the cellular energy-sensing pathways, which include AMP-activated protein kinase (AMPK) and sirtuins. By modulating these pathways, such compounds can promote the dephosphorylation and nuclear localization of FOXO1, thereby enhancing its transcriptional activity. Similarly, polyphenols like quercetin and epigallocatechin gallate may engage with signaling cascades linked to oxidative stress, potentially leading to an upsurge in FOXO1 expression. Other compounds such as lithium chloride, which inhibits GSK-3, and sodium butyrate, a histone deacetylase inhibitor, can also contribute to changes in the expression and activity of FOXO1 by altering its phosphorylation state or facilitating the transcriptional machinery's access to the FOXO1 promoter, respectively. These interactions underscore the complexity of cellular regulation and highlight the diverse mechanisms through which FOXO1 expression can be modulated by various molecules within the cell.

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