TY  - JOUR
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Metzler, Ralf
ED  - Metzler, Ralf
T1  - Kinetics of polymer looping with macromolecular crowding: effects of volume fraction and crowder size
JF  - Soft Matter
N2  - The looping of polymers such as DNA is a fundamental process in the molecular biology of living cells, whose interior is characterised by a high degree of molecular crowding. We here investigate in detail the looping dynamics of flexible polymer chains in the presence of different degrees of crowding. From the analysis of the looping–unlooping rates and the looping probabilities of the chain ends we show that the presence of small crowders typically slows down the chain dynamics but larger crowders may in fact facilitate the looping. We rationalise these non-trivial and often counterintuitive effects of the crowder size on the looping kinetics in terms of an effective solution viscosity and standard excluded volume. It is shown that for small crowders the effect of an increased viscosity dominates, while for big crowders we argue that confinement effects (caging) prevail. The tradeoff between both trends can thus result in the impediment or facilitation of polymer looping, depending on the crowder size. We also examine how the crowding volume fraction, chain length, and the attraction strength of the contact groups of the polymer chain affect the looping kinetics and hairpin formation dynamics. Our results are relevant for DNA looping in the absence and presence of protein mediation, DNA hairpin formation, RNA folding, and the folding of polypeptide chains under biologically relevant high-crowding conditions.
KW  - gene-regulation kinetics
KW  - physiological consequences
KW  - spatial-organization
KW  - anomalous diffusion
KW  - folding kinetics
KW  - living cells
KW  - dna coiling
KW  - in-vitro
KW  - dynamics
KW  - mixtures
Y1  - 2014
SN  - 1744-683X
SP  - 472
EP  - 488
PB  - The Royal Society of Chemistry
CY  - Cambridge
ER  - 
TY  - GEN
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Metzler, Ralf
T1  - Kinetics of polymer looping with macromolecular crowding: effects of volume fraction and crowder size
N2  - The looping of polymers such as DNA is a fundamental process in the molecular biology of living cells, whose interior is characterised by a high degree of molecular crowding. We here investigate in detail the looping dynamics of flexible polymer chains in the presence of different degrees of crowding. From the analysis of the looping–unlooping rates and the looping probabilities of the chain ends we show that the presence of small crowders typically slows down the chain dynamics but larger crowders may in fact facilitate the looping. We rationalise these non-trivial and often counterintuitive effects of the crowder size on the looping kinetics in terms of an effective solution viscosity and standard excluded volume. It is shown that for small crowders the effect of an increased viscosity dominates, while for big crowders we argue that confinement effects (caging) prevail. The tradeoff between both trends can thus result in the impediment or facilitation of polymer looping, depending on the crowder size. We also examine how the crowding volume fraction, chain length, and the attraction strength of the contact groups of the polymer chain affect the looping kinetics and hairpin formation dynamics. Our results are relevant for DNA looping in the absence and presence of protein mediation, DNA hairpin formation, RNA folding, and the folding of polypeptide chains under biologically relevant high-crowding conditions.
T3  - Zweitveröffentlichungen der Universität Potsdam : Mathematisch-Naturwissenschaftliche Reihe - 185 
KW  - gene-regulation kinetics
KW  - physiological consequences
KW  - spatial-organization
KW  - anomalous diffusion
KW  - folding kinetics
KW  - living cells
KW  - dna coiling
KW  - in-vitro
KW  - dynamics
KW  - mixtures
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-76961
SP  - 472
EP  - 488
PB  - The Royal Society of Chemistry
CY  - Cambridge
ER  - 
TY  - JOUR
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Kim, Won Kyu
A1  - Metzler, Ralf
T1  - Facilitation of polymer looping and giant polymer diffusivity in crowded solutions of active particles
JF  - New journal of physics : the open-access journal for physics
N2  - We study the dynamics of polymer chains in a bath of self-propelled particles (SPP) by extensive Langevin dynamics simulations in a two-dimensional model system. Specifically, we analyse the polymer looping properties versus the SPP activity and investigate how the presence of the active particles alters the chain conformational statistics. We find that SPPs tend to extend flexible polymer chains, while they rather compactify stiffer semiflexible polymers, in agreement with previous results. Here we show that higher activities of SPPs yield a higher effective temperature of the bath and thus facilitate the looping kinetics of a passive polymer chain. We explicitly compute the looping probability and looping time in a wide range of the model parameters. We also analyse the motion of a monomeric tracer particle and the polymer's centre of mass in the presence of the active particles in terms of the time averaged mean squared displacement, revealing a giant diffusivity enhancement for the polymer chain via SPP pooling. Our results are applicable to rationalising the dimensions and looping kinetics of biopolymers at constantly fluctuating and often actively driven conditions inside biological cells or in suspensions of active colloidal particles or bacteria cells.
KW  - diffusion
KW  - active transport
KW  - polymers
Y1  - 2015
U6  - https://doi.org/10.1088/1367-2630/17/11/113008
SN  - 1367-2630
VL  - 17
PB  - IOP Publ. Ltd.
CY  - Bristol
ER  - 
TY  - JOUR
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Metzler, Ralf
T1  - Mixing and segregation of ring polymers: spatial confinement and molecular crowding effects
JF  - New journal of physics : the open-access journal for physics
N2  - During the life cycle of bacterial cells the non-mixing of the two ring-shaped daughter genomes is an important prerequisite for the cell division process. Mimicking the environments inside highly crowded biological cells, we study the dynamics and statistical behavior of two flexible ring polymers in the presence of cylindrical confinement and crowding molecules. From extensive computer simulations we determine the degree of ring-ring overlap and the number of inter-monomer contacts for varying volume fractions phi of crowders. We also examine the entropic demixing of polymer rings in the presence of mobile crowders and determine the characteristic times of the internal polymer dynamics. Effects of the ring length on ring-ring overlap are also analyzed. In particular, on systematic variation of the fraction of crowding molecules, a (1 - phi)-scaling is found for the ring-ring overlap length along the cylinder axis, and a non-monotonic dependence of the 3D ring-ring contact number with a maximum at phi approximate to 0.2 is obtained. Our results demonstrate that polymer rings are demixed and separated by particular entropy-favourable partitioning of crowders along the axis of the cylindrical simulation box. These findings help to rationalize the implications of macromolecular crowding for circular DNA molecules in confined spaces inside bacteria as well as in localized cellular compartments inside eukaryotic cells.
KW  - polymers
KW  - confinement
KW  - crowding
Y1  - 2014
U6  - https://doi.org/10.1088/1367-2630/16/5/053047
SN  - 1367-2630
VL  - 16
PB  - IOP Publ. Ltd.
CY  - Bristol
ER  - 
TY  - JOUR
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Metzler, Ralf
T1  - Sensing viruses by mechanical tension of DNA in responsive hydrogels
JF  - Physical review : X, Expanding access
N2  - The rapid worldwide spread of severe viral infections, often involving novel mutations of viruses, poses major challenges to our health-care systems. This means that tools that can efficiently and specifically diagnose viruses are much needed. To be relevant for broad applications in local health-care centers, such tools should be relatively cheap and easy to use. In this paper, we discuss the biophysical potential for the macroscopic detection of viruses based on the induction of a mechanical stress in a bundle of prestretched DNA molecules upon binding of viruses to the DNA. We show that the affinity of the DNA to the charged virus surface induces a local melting of the double helix into two single-stranded DNA. This process effects a mechanical stress along the DNA chains leading to an overall contraction of the DNA. Our results suggest that when such DNA bundles are incorporated in a supporting matrix such as a responsive hydrogel, the presence of viruses may indeed lead to a significant, macroscopic mechanical deformation of the matrix. We discuss the biophysical basis for this effect and characterize the physical properties of the associated DNA melting transition. In particular, we reveal several scaling relations between the relevant physical parameters of the system. We promote this DNA-based assay as a possible tool for efficient and specific virus screening.
Y1  - 2014
U6  - https://doi.org/10.1103/PhysRevX.4.021002
SN  - 2160-3308
VL  - 4
IS  - 2
PB  - American Physical Society
CY  - College Park
ER  - 
TY  - JOUR
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Metzler, Ralf
T1  - Self-subdiffusion in solutions of star-shaped crowders: non-monotonic effects of inter-particle interactions
JF  - New journal of physics : the open-access journal for physics
N2  - We examine by extensive computer simulations the self-diffusion of anisotropic star-like particles in crowded two-dimensional solutions. We investigate the implications of the area coverage fraction phi of the crowders and the crowder-crowder adhesion properties on the regime of transient anomalous diffusion. We systematically compute the mean squared displacement (MSD) of the particles, their time averaged MSD, and the effective diffusion coefficient. The diffusion is ergodic in the limit of long traces, such that the mean time averaged MSD converges towards the ensemble averaged MSD, and features a small residual amplitude spread of the time averaged MSD from individual trajectories. At intermediate time scales, we quantify the anomalous diffusion in the system. Also, we show that the translational-but not rotational-diffusivity of the particles Dis a nonmonotonic function of the attraction strength between them. Both diffusion coefficients decrease as the power law D(phi) similar to (1 - phi/phi*)(2 ... 2.4) with the area fraction phi occupied by the crowders and the critical value phi*. Our results might be applicable to rationalising the experimental observations of non-Brownian diffusion for a number of standard macromolecular crowders used in vitro to mimic the cytoplasmic conditions of living cells.
KW  - anomalous diffusion
KW  - crowded fluids
KW  - stochastic processes
Y1  - 2015
U6  - https://doi.org/10.1088/1367-2630/17/11/113028
SN  - 1367-2630
VL  - 17
PB  - IOP Publ. Ltd.
CY  - Bristol
ER  - 
TY  - JOUR
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Metzler, Ralf
T1  - Kinetics of polymer looping with macromolecular crowding: effects of volume fraction and crowder size
JF  - Soft matter
N2  - The looping of polymers such as DNA is a fundamental process in the molecular biology of living cells, whose interior is characterised by a high degree of molecular crowding. We here investigate in detail the looping dynamics of flexible polymer chains in the presence of different degrees of crowding. From the analysis of the looping-unlooping rates and the looping probabilities of the chain ends we show that the presence of small crowders typically slows down the chain dynamics but larger crowders may in fact facilitate the looping. We rationalise these non-trivial and often counterintuitive effects of the crowder size on the looping kinetics in terms of an effective solution viscosity and standard excluded volume. It is shown that for small crowders the effect of an increased viscosity dominates, while for big crowders we argue that confinement effects (caging) prevail. The tradeoff between both trends can thus result in the impediment or facilitation of polymer looping, depending on the crowder size. We also examine how the crowding volume fraction, chain length, and the attraction strength of the contact groups of the polymer chain affect the looping kinetics and hairpin formation dynamics. Our results are relevant for DNA looping in the absence and presence of protein mediation, DNA hairpin formation, RNA folding, and the folding of polypeptide chains under biologically relevant high-crowding conditions.
Y1  - 2015
U6  - https://doi.org/10.1039/c4sm02007c
SN  - 1744-683X
SN  - 1744-6848
VL  - 11
IS  - 3
SP  - 472
EP  - 488
PB  - Royal Society of Chemistry
CY  - Cambridge
ER  - 
TY  - JOUR
A1  - Shin, Jaeoh
A1  - Cherstvy, Andrey G.
A1  - Metzler, Ralf
T1  - Polymer looping is controlled by macromolecular crowding, spatial confinement, and chain stiffness
JF  - ACS Macro Letters
N2  - We study by extensive computer simulations the looping characteristics of linear polymers with varying persistence length inside a spherical cavity in the presence of macromolecular crowding. For stiff chains, the looping probability and looping time reveal wildly oscillating patterns as functions of the chain length. The effects of crowding differ dramatically for flexible versus stiff polymers. While for flexible chains the looping kinetics is slowed down by the crowders, for stiffer chains the kinetics turns out to be either decreased or facilitated, depending on the polymer length. For severe confinement, the looping kinetics may become strongly facilitated by crowding. Our findings are of broad impact for DNA looping in the crowded and compartmentalized interior of living biological cells.
Y1  - 2015
U6  - https://doi.org/10.1021/mz500709w
SN  - 2161-1653
VL  - 4
IS  - 2
SP  - 202
EP  - 206
PB  - American Chemical Society
CY  - Washington
ER  -