Date published: 2025-9-11

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Histone H3.3B Inhibitors

Histone H3.3B is one of the variants of the H3 histone family, integral components of the nucleosome structure in eukaryotic cells. Histones are fundamental to the organization of DNA within the nucleus, facilitating its compaction into chromatin and playing pivotal roles in gene regulation. The H3 family, in particular, has been the focus of extensive research due to its post-translational modifications, such as methylation, acetylation, and phosphorylation. These modifications, often occurring at the N-terminal tail of the histone, serve as epigenetic marks, dictating the transcriptional state of associated genes. Histone H3.3B, as a variant, has specific sequence differences from the canonical H3 histones and is incorporated into chromatin independent of DNA replication. This unique incorporation pattern allows H3.3B to be involved in specific cellular processes, such as the maintenance of chromatin structure during transcription, DNA repair, and the formation of heterochromatin.

Inhibitors of Histone H3.3B aim to modulate the function of this histone variant, primarily by targeting its post-translational modifications or its chaperones responsible for its deposition onto DNA. By altering the modification state or deposition pattern of H3.3B, these inhibitors can impact the chromatin landscape and consequently, gene expression patterns within the cell. For instance, an inhibitor that prevents the acetylation of H3.3B might promote a more condensed chromatin state, leading to gene silencing. Conversely, an inhibitor that enhances such acetylation could lead to a more relaxed chromatin structure and enhanced gene transcription. It's crucial to understand that these inhibitors, by virtue of targeting a fundamental aspect of cell biology, alter a wide array of cellular processes. The specificity, potency, and mode of action of each inhibitor determine its effect on H3.3B's function and, by extension, on chromatin dynamics and gene regulation.

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