Date published: 2025-9-22

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Egr-1 Inhibitors

Egr-1 inhibitors represent a diverse and intriguing class of chemical compounds that have garnered significant attention in the field of molecular biology and cellular research. Egr-1, short for Early Growth Response protein 1, is a transcription factor that plays a crucial role in modulating gene expression in response to various stimuli. Its intricate involvement in cellular processes such as proliferation, differentiation, and stress response has made it an attractive target for scientific investigation. Egr-1 inhibitors are designed to specifically interact with and regulate the activity of this transcription factor. These inhibitors encompass a wide range of chemical classes, each possessing unique structural features and mechanisms of action. Some of the commonly studied Egr-1 inhibitors include small molecules, natural compounds, and synthetic derivatives. Triptolide has been recognized for its ability to interfere with Egr-1's function by inhibiting its DNA-binding activity. Similarly, epigallocatechin gallate (EGCG), a polyphenol found abundantly in green tea, has been shown to modulate Egr-1 expression through its impact on upstream signaling pathways. In addition to natural compounds, several synthetic Egr-1 inhibitors have been developed through extensive chemistry efforts. These synthetic compounds often exhibit increased specificity and potency compared to their natural counterparts. Researchers have explored diverse structural scaffolds to fine-tune the inhibitory activity of these compounds and their interaction with Egr-1. While the exact mechanisms of action may vary, Egr-1 inhibitors predominantly function by disrupting the transcription factor's binding to specific DNA sequences or by interfering with its interactions with coactivators and other regulatory proteins. This, in turn, modulates the expression of genes downstream of Egr-1, affecting various cellular pathways and biological responses.

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