A fine kinetic balance of interactions directs transcription factor hubs to genes.
Apratim MukherjeeSamantha FallacaroPuttachai RatchasanmuangJoseph ZinskiAlan BokaKareena ShanktaMustafa MirPublished in: bioRxiv : the preprint server for biology (2024)
Eukaryotic gene regulation relies on the binding of sequence-specific transcription factors (TFs). TFs bind chromatin transiently yet occupy their target sites by forming high-local concentration microenvironments (hubs and condensates) that increase the frequency of binding events. Despite their ubiquity, such microenvironments have been difficult to study in endogenous contexts due to technical limitations. Here, we overcome these limitations and investigate how hubs drive TF occupancy at their targets. Using a DNA binding perturbation to a hub-forming TF, Zelda, in Drosophila embryos, we find that hub properties, including the stability and frequencies of associations to targets, are key determinants of TF occupancy. Our data suggest that the targeting of these hubs is driven not just by specific DNA motif recognition, but also by a fine-tuned kinetic balance of interactions between TFs and their co-binding partners.
Keyphrases
- dna binding
- transcription factor
- genome wide identification
- air pollution
- bioinformatics analysis
- genome wide
- circulating tumor
- dna damage
- cancer therapy
- big data
- gene expression
- cell free
- single molecule
- oxidative stress
- artificial intelligence
- machine learning
- hepatitis c virus
- amino acid
- data analysis
- nucleic acid
- men who have sex with men