Date published: 2025-10-13

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JMJD3 Activators

JMJD3 Activators include compounds that increase the activity of the histone demethylase JMJD3. These compounds are not activators in the traditional sense, as they do not bind directly to JMJD3 and stimulate its activity. Instead, they may influence cellular processes and pathways that result in the upregulation of JMJD3 or in an increase in its substrate availability. The mechanisms by which these compounds are thought to act are diverse, and they may affect JMJD3 through genomic and non-genomic pathways, enzyme stabilization, or through alterations in cellular metabolites that are necessary for the catalytic activity of JMJD3.

For instance, compounds like 5-Aza-2'-deoxycytidine and vitamin C can induce global changes in DNA and histone methylation status, which may lead to an upregulated expression or enhanced activity of JMJD3. Other compounds, such as retinoic acid and sulforaphane, may act through modulation of gene expression, resulting in increased levels of JMJD3. Additionally, dietary components like genistein, resveratrol, and epigallocatechin gallate, through their influence on various cell signaling and epigenetic pathways, could indirectly enhance JMJD3 activity. The role of these compounds in modulating JMJD3 activity is not direct but is instead a consequence of their broader impact on cellular homeostasis and gene regulation networks. While the idea of activating JMJD3 via small molecules remains largely theoretical, the study of these compounds provides valuable insights into the complex regulation of epigenetic enzymes and the interplay between different types of epigenetic modifications. Understanding how these compounds can indirectly affect JMJD3 activity can contribute to the broader field of epigenetics and gene regulation.

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