Enhanced Preprints

Local Volume Concentration, Packing Domains and Scaling Properties of Chromatin

  1. Marcelo Carignano
  2. Martin Kröger
  3. Luay Matthew Almassalha
  4. Vasundhara Agrawal
  5. Wing Shun Li
  6. Emily M. Pujadas-Liwag
  7. Rikkert J. Nap
  8. Vadim Backman
  9. Igal Szleifer author has email address
  1. Department of Biomedical Engineering, Northwestern University, Evanston, IL 60208, USA
  2. Magnetism and Interface Physics & Computational Polymer Physics, Department of Materials, ETH Zurich, CH-8093 Zurich, Switzerland
  3. Department of Gastroenterology and Hepatology, Northwestern Memorial Hospital, Chicago IL 60611, USA
  4. Applied Physics Program, Northwestern University, Evanston, IL 60208, USA
  5. Department of Chemistry, Northwestern University, Evanston, IL 60208, USA

Peer review process

Not revised: This Reviewed Preprint includes the authors’ original preprint (without revision), an eLife assessment, public reviews, and a response from the authors (if available).

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Editors

  • Reviewing Editor
    Bin Zhang
    Massachusetts Institute of Technology, Cambridge, United States of America
  • Senior Editor
    Felix Campelo
    Institute of Photonic Sciences, Barcelona, Spain

Reviewer #1 (Public Review):

Carignano et al propose an extension of the self-returning random walk (SRRW) model for chromatin to include excluded volume aspects and use it to investigate generic local and global properties of the chromosome 3D organization inside eukaryotic nuclei. In particular, they focus on chromatin volumic density, contact probability, and domain size and suggest that their framework can recapitulate several experimental observations and predict the effect of some perturbations.

Strengths:

• The developed methodology is convincing and may offer an alternative - less computationally demanding - framework to investigate the single-cell and population structural properties of 3D genome organization at multiple scales.

• Compared to the previous SRRW model, it allows for investigation of the role of excluded volume locally.

• They perform some experiments to compare with model predictions and show consistency between the two.

Weaknesses:

• The model is a homopolymer model and currently cannot fully account for specific mechanisms that may shape the heterogeneous, complex organization of chromosomes (TAD at specific positions, A/B compartmentalization, promoter-enhancer loops, etc.).

• By construction of their framework, the effect of excluded volume is only local and larger-scale properties for which excluded volume could be a main actor (formation of chromosome territories [Rosa & Everaers, PLoS CB 2009], bottle-brush effects due to loop extrusion [Polovnikov et al, PRX 2023], etc.) cannot be captured.

• Apart from being a computationally interesting approach to generating realistic 3D chromosome organization, the method offers fewer possibilities than standard polymer models (eg, MD simulations) of chromatin (no dynamics, no specific mechanisms, etc.) with likely the same predictive power under the same hypotheses. In particular, authors often claim the superiority of their approach to describing the local chromatin compaction compared to previous polymer models without showing it or citing any relevant references that would show it.

• Comparisons with experiments are solid but are not quantified.

Impact:

Building on the presented framework in the future to incorporate TAD and compartments may offer an interesting model to study the single-cell heterogeneity of chromatin organization. But currently, in this reviewer's opinion, standard polymer modeling frameworks may offer more possibilities.

Reviewer #2 (Public Review):

Summary:

The authors introduce a simple Self Returning Excluded Volume (SR-EV) model to investigate the 3D organization of chromatin. This is a random walk with a probability to self-return accounting for the excluded volume effects. The authors use this method to study the statistical properties of chromatin organization in 3D. They compute contact probabilities, 3D distances, and packing properties of chromatin and compare them with a set of experimental data.

Strengths:

(1) Typically, to generate a polymer with excluded volume interactions, one needs to run long simulations with computationally expensive repulsive potentials like the Weeks-Chanlder-Anderson potential. However, here, instead of performing long simulations, the authors have devised a method where they can grow polymer, enabling quick generation of configurations.

(2) Authors show that the chromatin configurations generated from their models do satisfy many of the experimentally known statistical properties of chromatin. Contact probability scalings and packing properties are comparable with Chromatin Scanning Transmission Electron Microscopy (ChromSTEM) experimental data from some of the cell types.

Weaknesses:

This can only generate broad statistical distributions. This method cannot generate sequence-dependent effects, specific TAD structures, or compartments without a prior model for the folding parameter alpha. It cannot generate a 3D distance between specific sets of genes. This is an interesting soft-matter physics study. However, the output is only as good as the alpha value one provides as input.

  1. Howard Hughes Medical Institute
  2. Wellcome Trust
  3. Max-Planck-Gesellschaft
  4. Knut and Alice Wallenberg Foundation