LELP1 Inhibitors are a diverse set of chemical compounds that target various components and regulatory mechanisms of the Hedgehog (Hh) signaling pathway, which is essential for LELP1's functional activity. Cyclopamine and Jervine, by binding to and inhibiting Smoothened (SMO), a critical transmembrane protein in the Hh pathway, lead to the downregulation of LELP1 due to the pathway's impairment. Other SMO antagonists like Vismodegib, Erismodegib, and Saridegib, function through a similar mechanism, suppressing the pathway's activity and subsequent LELP1 function. Further along the pathway, GANT61 specifically targets and inhibits GLI transcription factors, which are downstream effectors in the Hh signaling, thereby reducing the transcriptional activation of LELP1. The antifungal Itraconazole, albeit originally intended for a different application, also inhibits SMO, showcasing the pathway's vulnerability to a broad range of compounds, and in turn affecting LELP1 activity.
Additional chemicals exert their inhibitory effects on LELP1 by modulating the biosynthesis and trafficking of pathway components or through indirect suppression of the Hh pathway. Fluvastatin, a cholesterol-lowering agent, and U 18666A, a disruptor of cholesterol homeostasis, both decrease the bioavailability of lipids necessary for the post-translational modification of Hh ligands, thereby reducing LELP1 functionality. Cholecalciferol suppresses Hh signaling through multiple mechanisms, leading to diminished LELP1 expression and activity. Tolfenamic acid, although primarily an anti-inflammatory drug, has been found to impede GLI activity, which is crucial forthe Hh pathway's function and consequently LELP1's role. Lastly, Arsenic(III) oxide, a compound with various cellular targets, degrades GLI proteins, further contributing to the attenuation of LELP1 due to decreased Hh pathway signaling. Collectively, these LELP1 Inhibitors, through their targeted disruption of the Hh signaling cascade, serve to diminish the functional activity of LELP1 without affecting its transcription or translation directly.
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