Protein motion in the nucleus: from anomalous diffusion to weak interactions
Maxime Woringer, Xavier Darzacq

TL;DR
This paper reviews how transcription factors diffuse in the nucleus, linking anomalous diffusion to weak, transient interactions with nuclear structures, and suggests improved analysis methods for single-particle tracking data.
Contribution
It proposes that anomalous diffusion of transcription factors results from weak, transient interactions with nuclear substructures and highlights the need for better SPT data analysis methods.
Findings
Anomalous diffusion reflects transient interactions in the nucleus.
Nuclear organization influences transcription factor dynamics.
Improved SPT analysis can reveal nuclear substructure interactions.
Abstract
Understanding how transcription factors (TFs) regulate mammalian gene expression in space and time is a central topic in biology. To activate a gene, a TF has first to diffuse in the available space of the nucleus until it reaches a target DNA sequence or protein (target site). This eventually results in the recruitment of the whole transcriptional machinery. All these processes take place in the mammalian nucleoplasm, a highly organized and dynamic environment, in which some complexes transiently assemble and break apart, whereas others appear more stable. This diversity of dynamic behaviors arises from the number of biomolecules that make up the nucleoplasm and their pairwise interactions. Indeed, interactions energies that span several orders of magnitude, from covalent bounds to transient and dynamic interactions can shape nuclear landscapes. Thus, the nuclear environment…
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