Your search keyword '"Krepel D"' showing total 8 results

1. Towards graphene based ultrasensitive chemical detectors: Lithium anchoring of organic molecules on the surface of graphene

Author

Krepel, D., primary and Hod, O., additional

Published

2013

2. Braiding topology and the energy landscape of chromosome organization proteins.

Author

Krepel D, Davtyan A, Schafer NP, Wolynes PG, and Onuchic JN

Subjects

Binding Sites, Chromosomal Proteins, Non-Histone metabolism, Humans, Kinesins metabolism, Protein Binding, Chromosomal Proteins, Non-Histone chemistry, Kinesins chemistry, Molecular Dynamics Simulation

Abstract

Assemblies of structural maintenance of chromosomes (SMC) proteins and kleisin subunits are essential to chromosome organization and segregation across all kingdoms of life. While structural data exist for parts of the SMC-kleisin complexes, complete structures of the entire complexes have yet to be determined, making mechanistic studies difficult. Using an integrative approach that combines crystallographic structural information about the globular subdomains, along with coevolutionary information and an energy landscape optimized force field (AWSEM), we predict atomic-scale structures for several tripartite SMC-kleisin complexes, including prokaryotic condensin, eukaryotic cohesin, and eukaryotic condensin. The molecular dynamics simulations of the SMC-kleisin protein complexes suggest that these complexes exist as a broad conformational ensemble that is made up of different topological isomers. The simulations suggest a critical role for the SMC coiled-coil regions, where the coils intertwine with various linking numbers. The twist and writhe of these braided coils are coupled with the motion of the SMC head domains, suggesting that the complexes may function as topological motors. Opening, closing, and translation along the DNA of the SMC-kleisin protein complexes would allow these motors to couple to the topology of DNA when DNA is entwined with the braided coils., Competing Interests: The authors declare no competing interest.

Published

2020

3. Deciphering the structure of the condensin protein complex.

Author

Krepel D, Cheng RR, Di Pierro M, and Onuchic JN

Subjects

Adenosine Triphosphatases metabolism, Amino Acid Sequence, Bacterial Proteins metabolism, Bacterial Proteins physiology, Cell Cycle Proteins metabolism, Cell Cycle Proteins physiology, Chromosomal Proteins, Non-Histone metabolism, Chromosome Segregation physiology, Chromosomes metabolism, DNA-Binding Proteins metabolism, Databases, Protein, Multiprotein Complexes metabolism, Nuclear Proteins metabolism, Protein Domains, Structure-Activity Relationship, Adenosine Triphosphatases physiology, Adenosine Triphosphatases ultrastructure, DNA-Binding Proteins physiology, DNA-Binding Proteins ultrastructure, Multiprotein Complexes physiology, Multiprotein Complexes ultrastructure

Abstract

Protein assemblies consisting of structural maintenance of chromosomes (SMC) and kleisin subunits are essential for the process of chromosome segregation across all domains of life. Prokaryotic condensin belonging to this class of protein complexes is composed of a homodimer of SMC that associates with a kleisin protein subunit called ScpA. While limited structural data exist for the proteins that comprise the (SMC)-kleisin complex, the complete structure of the entire complex remains unknown. Using an integrative approach combining both crystallographic data and coevolutionary information, we predict an atomic-scale structure of the whole condensin complex, which our results indicate being composed of a single ring. Coupling coevolutionary information with molecular-dynamics simulations, we study the interaction surfaces between the subunits and examine the plausibility of alternative stoichiometries of the complex. Our analysis also reveals several additional configurational states of the condensin hinge domain and the SMC-kleisin interaction domains, which are likely involved with the functional opening and closing of the condensin ring. This study provides the foundation for future investigations of the structure-function relationship of the various SMC-kleisin protein complexes at atomic resolution., Competing Interests: The authors declare no conflict of interest.

Published

2018

4. Intersegmental transfer of proteins between DNA regions in the presence of crowding.

Author

Krepel D and Levy Y

Subjects

DNA chemistry, Diffusion, Kinetics, DNA-Binding Proteins chemistry, Models, Molecular

Abstract

Intersegmental transfer that involves direct relocation of a DNA-binding protein from one nonspecific DNA site to another was previously shown to contribute to speeding up the identification of the DNA target site. This mechanism is promoted when the protein is composed of at least two domains that have different DNA binding affinities and thus show a degree of mobility. In this study, we investigate the effect of particle crowding on the ability of a multi-domain protein to perform intersegmental transfer. We show that although crowding conditions often favor 1D diffusion of proteins along DNA over 3D diffusion, relocation of one of the tethered domains to initiate intersegmental transfer is possible even under crowding conditions. The tendency to perform intersegmental transfer by a multi-domain protein under crowding conditions is much higher for larger crowding particles than smaller ones and can be even greater than under no-crowding conditions. We report that the asymmetry of the two domains is even magnified by the crowders. The observations that crowding supports intersegmental transfer serve as another example that in vivo complexity does not necessarily slow down DNA search kinetics by proteins.

Published

2017

5. Mechanism of Facilitated Diffusion during a DNA Search in Crowded Environments.

Author

Krepel D, Gomez D, Klumpp S, and Levy Y

Subjects

Diffusion, Kinetics, Monte Carlo Method, DNA chemistry, Molecular Dynamics Simulation

Abstract

The key feature explaining the rapid recognition of a DNA target site by its protein lies in the combination of one- and three-dimensional (1D and 3D) diffusion, which allows efficient scanning of the many alternative sites. This facilitated diffusion mechanism is expected to be affected by cellular conditions, particularly crowding, given that up to 40% of the total cellular volume may by occupied by macromolecules. Using coarse-grained molecular dynamics and Monte Carlo simulations, we show that the crowding particles can enhance facilitated diffusion and accelerate search kinetics. This effect originates from a trade-off between 3D and 1D diffusion. The 3D diffusion coefficient is lower under crowded conditions, but it has little influence because the excluded volume effect of molecular crowding restricts its use. Largely prevented from using 3D diffusion, the searching protein dramatically increases its use of the hopping search mode, which results in a higher linear diffusion coefficient. The coefficient of linear diffusion also increases under crowded conditions as a result of increased collisions between the crowding particles and the searching protein. Overall, less 3D diffusion coupled with an increase in the use of the hopping and speed of 1D diffusion results in faster search kinetics under crowded conditions. Our study shows that the search kinetics and mechanism are modulated not only by the crowding occupancy but also by the properties of the crowding particles and the salt concentration.

Published

2016

6. Effects of Edge Oxidation on the Structural, Electronic, and Magnetic Properties of Zigzag Boron Nitride Nanoribbons.

Author

Krepel D and Hod O

Abstract

The effects of edge chemistry on the relative stability and electronic properties of zigzag boron nitride nanoribbons (ZBNNRs) are investigated. Among all functional groups considered, fully hydroxylated ZBNNRs are found to be the most energetically stable. When an in-plane external electric field is applied perpendicular to the axis of both hydrogenated and hydroxylated ZBNNRs, a spin-polarized half-metallic state is induced, whose character is different than that predicted for zigzag graphene nanoribbons. The onset field for achieving the half-metallic state is found to mainly depend on the width of the ribbon. Our results indicate that edge functionalization of ZBNNRs may open the way for the design of new nanoelectronic and nanospintronic devices.

Published

2014

7. Robust Superlubricity in Graphene/h-BN Heterojunctions.

Author

Leven I, Krepel D, Shemesh O, and Hod O

Abstract

The sliding energy landscape of the heterogeneous graphene/h-BN interface is studied by means of the registry index. For a graphene flake sliding on top of h-BN, the anisotropy of the sliding energy corrugation with respect to the misfit angle between the two naturally mismatched lattices is found to reduce with the flake size. For sufficiently large flakes, the sliding energy corrugation is expected to be at least an order of magnitude lower than that obtained for matching lattices regardless of the relative interlayer orientation. Therefore, in contrast to the case of the homogeneous graphene interface where flake reorientations are known to eliminate superlubricty, here, a stable low-friction state is expected to occur. Our results mark heterogeneous layered interfaces as promising candidates for dry lubrication purposes.

Published

2013

8. Protective effects of neurotrophic factor-secreting cells in a 6-OHDA rat model of Parkinson disease.

Author

Sadan O, Bahat-Stromza M, Barhum Y, Levy YS, Pisnevsky A, Peretz H, Ilan AB, Bulvik S, Shemesh N, Krepel D, Cohen Y, Melamed E, and Offen D

Subjects

Animals, Behavior, Animal drug effects, Cells, Cultured, Disease Models, Animal, Humans, Magnetic Resonance Imaging, Male, Oxidopamine, Parkinson Disease pathology, Rats, Rats, Sprague-Dawley, Mesenchymal Stem Cells metabolism, Nerve Growth Factors metabolism, Parkinson Disease metabolism, Parkinson Disease therapy, Stem Cell Transplantation

Abstract

Stem cell-based therapy is a promising treatment for neurodegenerative diseases. In our laboratory, a novel protocol has been developed to induce bone marrow-derived mesenchymal stem cells (MSC) into neurotrophic factors- secreting cells (NTF-SC), thus combining stem cell-based therapy with the NTF-based neuroprotection. These cells produce and secrete factors such as brain-derived neurotrophic factor (BDNF) and glial cell-derived neurotrophic factor. Conditioned medium of the NTF-SC that was applied to a neuroblastoma cell line (SH-SY5Y) 1 h before exposure to the neurotoxin 6-hydroxydopamine (6-OHDA) demonstrated marked protection. An efficacy study was conducted on the 6-OHDA-induced lesion, a rat model of Parkinson's disease. The cells, either MSC or NTF-SC, were transplanted on the day of 6-OHDA administration and amphetamine-induced rotations were measured as a primary behavior index. We demonstrated that when transplanted posterior to the 6-OHDA lesion, the NTF-SC ameliorated amphetamine-induced rotations by 45%. HPLC analysis demonstrated that 6-OHDA induced dopamine depletion to a level of 21% compared to the untreated striatum. NTF-SC inhibited dopamine depletion to a level of 72% of the contralateral striatum. Moreover, an MRI study conducted with iron-labeled cells, followed by histological verification, revealed that the engrafted cells migrated toward the lesion. In a histological assessment, we found that the cells induced regeneration in the damaged striatal dopaminergic nerve terminal network. We therefore conclude that the induced MSC have a therapeutic potential for neurodegenerative processes and diseases, both by the NTFs secretion and by the migratory trait toward the diseased tissue.

Published

2009