4.2 Article

Cyclic-polymer grafted colloids in spherical confinement: insights for interphase chromosome organization

Journal

PHYSICAL BIOLOGY
Volume 20, Issue 5, Pages -

Publisher

IOP Publishing Ltd
DOI: 10.1088/1478-3975/ace750

Keywords

chromosome organization; cyclic polymers; molecular simulations; colloidal particles

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Through extensive coarse-grained simulations, we modeled interphase chromosome structures as colloidal particles grafted with cyclic polymers. These simulations revealed that the polymer-grafted colloidal system can provide well-separated particle distribution without specific attraction between the chain monomers. The results also showed that the organization of chromosomal regions can be altered by varying the polymerization degree and introducing DNA breaks, providing insights into the 3D genome architecture.
Interphase chromosomes are known to organize non-randomly in the micron-sized eukaryotic cell nucleus and occupy certain fraction of nuclear volume, often without mixing. Using extensive coarse-grained simulations, we model such chromosome structures as colloidal particles whose surfaces are grafted by cyclic polymers. This model system is known as Rosetta. The cyclic polymers, with varying polymerization degrees, mimic chromatin loops present in interphase chromosomes, while the rigid core models the chromocenter section of the chromosome. Our simulations show that the colloidal chromosome model provides a well-separated particle distribution without specific attraction between the chain monomers. As the polymerization degree of the grafted cyclic chains decreases while maintaining the total chromosomal length (e.g. the more potent activity of condensin-family proteins), the average chromosomal volume becomes smaller, inter-chromosomal contacts decrease, and chromocenters organize in a quasi-crystalline order reminiscent of a glassy state. This order weakens for polymer chains with a characteristic size on the order of the confinement radius. Notably, linear-polymer grafted particles also provide the same chromocenter organization scheme. However, unlike linear chains, cyclic chains result in less contact between the polymer layers of neighboring chromosome particles, demonstrating the effect of DNA breaks in altering genome-wide contacts. Our simulations show that polymer-grafted colloidal systems could help decipher 3D genome architecture along with the fractal globular and loop-extrusion models.

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