Date published: 2025-10-26

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NDRG1 Inhibitors

NDRG1 inhibitors comprise a diverse set of compounds that indirectly modulate the activity or expression of the NDRG1 protein. These inhibitors exert their effects through various mechanisms and signaling pathways that intersect with the regulation and function of NDRG1. Compounds such as staurosporine and sorafenib have multi-target effects on kinases that are part of signaling cascades relevant to NDRG1's regulation. By inhibiting these kinases, these compounds can modulate the phosphorylation state of NDRG1, which is essential for its function. Agents like Trichostatin A and 2-Deoxy-D-glucose alter the cellular environment and gene expression in a way that impacts the regulation of NDRG1. Histone deacetylase inhibition by Trichostatin A changes the expression of a wide array of genes, including those governing NDRG1 expression, while 2-DG disrupts energy metabolism, which could affect NDRG1 stability and turnover. On the other hand, compounds like PIK-75, LY294002, and rapamycin disrupt the PI3K/AKT/mTOR pathway, which is pivotal for the regulation of cell survival and metabolism, processes that are known to influence NDRG1 expression and function. Moreover, natural compounds such as quercetin and curcumin are known for their broad spectrum of biological activities, including modulation of cell proliferation, survival pathways, and transcription factors, all of which can lead to changes in NDRG1 dynamics. In the context of NDRG1 regulation, these compounds can alter signaling pathways or transcriptional programs that either suppress or promote the expression of NDRG1. The ability these compounds to inhibit NDRG1 activity stems from their capacity to interfere with the complex regulatory networks that control NDRG1's role in cell stress responses, differentiation, and metabolism. Each of these compounds, although not directly interacting with NDRG1, can influence the protein's function through the interconnected web of cellular signaling.

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