Histone H3 (mono methyl Lys4) Antibody

About the Target

Histone H3 mono-methylation at lysine 4 (H3K4me1) is a post-translational modification marking enhancer regions involved in gene regulation. Histone H3, a core component of the nucleosome, has an N-terminal tail where lysine 4 (K4) resides, enabling modifications like mono-methylation. This modification is catalyzed by SET domain-containing methyltransferases, such as those in the SET1/MLL complexes, and is reversible by demethylases like LSD1. Depending on the literature source, Histone H3 may also be discussed as Histone H3 (mono methyl Lys4) and Histone H3 (mono methyl K4).

Reported cellular context includes chromosome, nucleosome core, and nucleus, which can matter when signal is compared across treatments or changing cell states. Following Histone H3 across matched perturbations can help separate abundance effects from shifts in localization, complex assembly, or pathway state.

Research Context

Histone H3 is commonly interpreted in the context of epigenetics research, and readouts are often stronger when a study separates expression changes from compartment-level redistribution. When reported signal spans chromosome, nucleosome core, and nucleus, a defined reference condition can make comparisons more interpretable across perturbations, passages, or replicate sets.

Consider these angles when interpreting target-level changes:

• apparent redistribution between chromosome, nucleosome core, and nucleus across matched conditions
• links between target behavior and transcriptional or chromatin-state changes
• differences between total target abundance and site-specific regulation when modified forms are compared
• co-patterning with orthogonal markers and control conditions that clarify pathway state

Variant Considerations

If your project spans exploratory questions, the regular version offers a balanced option for establishing baseline signal behavior for Histone H3. This can help when protocols evolve over time and the goal is to compare experiments using a stable reference workflow.

Standardize sampling time, control choice, and downstream analysis thresholds so apparent differences in Histone H3 reflect biology rather than handling. When interpreting Histone H3, it is often useful to decide early whether the main question is overall abundance, compartmental enrichment, or context-dependent redistribution.

For multi-run studies, a shared reference condition can keep Histone H3 trends easier to compare across datasets. That kind of consistency is especially helpful when follow-up work expands to new perturbations, model systems, or longitudinal collections.