Date published: 2025-11-5

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TXNDC15 Inhibitors

TXNDC15 inhibitors function by modulating specific cellular pathways and biochemical reactions that govern the protein's synthesis, post-translational modification, and degradation. For example, Trichostatin A acts as a HDAC inhibitor, impairing histone deacetylation, which affects the DNA binding affinity of the promoter region governing TXNDC15. The altered chromatin state impacts transcription, thereby reducing the synthesis of TXNDC15. 5-Azacytidine, on the other hand, targets the DNA methylation status of the promoter region and consequently restricts the expression of TXNDC15. In the realm of cellular signaling, LY294002 and Wortmannin operate as PI3K inhibitors, interrupting the PI3K-AKT pathway. By doing so, these chemicals affect the post-translational modification of TXNDC15, ultimately affecting its functionality.

The focus also extends to chemicals like Rapamycin, which inhibit mTOR pathways and therefore suppress the synthesis of the protein. Similarly, Bortezomib inhibits the proteasome, thereby affecting the degradation pathways for proteins that may regulate TXNDC15 negatively, causing an accumulation of such proteins and resulting in TXNDC15 inhibition. Auranofin provides a direct approach, inhibiting thioredoxin reductase and interfering with the redox regulation of TXNDC15. Nutlin-3 enhances the functionality of p53, a protein that promotes the degradation of TXNDC15. In this way, various inhibitors, either directly or indirectly, lead to the effective inhibition of TXNDC15 without affecting unrelated cellular processes.

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