Date published: 2025-10-30

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4933421E11Rik Inhibitors

The chemical class Lrif1 Inhibitors encompasses a range of compounds that can indirectly influence the function of Lrif1 through modulation of nuclear receptor signaling, alteration of kinase activity, or disruption of cellular protein homeostasis. These inhibitors are not unified by a common chemical structure or target but are connected through their capacity to affect cellular pathways that Lrif1 is likely to interact with or regulate.

For instance, Tamoxifen and Bicalutamide modulate the activity of estrogen and androgen receptors, respectively, which are central to the regulatory networks that Lrif1 may be a part of due to its role as a nuclear receptor interacting protein. Similarly, compounds like GW501516 and T0901317 can influence peroxisome proliferator-activated receptors, potentially altering the signaling context in which Lrif1 operates. Inhibitors such as LY294002 and PD98059 target key kinases within prominent signaling cascades like PI3K/AKT and MAPK/ERK, pathways that can intersect with the regulatory mechanisms involving Lrif1. Trichostatin A and 5-Azacytidine affect chromatin structure and DNA methylation, respectively, thereby modulating gene expression patterns that can include Lrif1-regulated genes. MG132 and Chloroquine disrupt proteostasis, affecting protein degradation systems that can control Lrif1 levels within the cell, while Rosiglitazone's activity on PPARγ signaling may have downstream effects on Lrif1's regulatory functions.

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