Your search keyword '"Miran Liber"' showing total 6 results

1. Developing DNA Nanotechnology Using Single-Molecule Fluorescence

Author

Eyal Nir, Roman Tsukanov, Miran Liber, Yaron Berger, and Toma E. Tomov

Subjects

chemistry.chemical_classification, DNA, Cruciform, Computer science, Lasers, Biomolecule, Immobilized Nucleic Acids, Nanotechnology, Context (language use), DNA, General Medicine, General Chemistry, Single-molecule experiment, Fluorescence, Diffusion, Kinetics, Förster resonance energy transfer, chemistry, DNA nanotechnology, Fluorescence Resonance Energy Transfer, Holliday junction, Nucleic Acid Conformation, DNA origami, A-DNA

Abstract

CONSPECTUS: An important effort in the DNA nanotechnology field is focused on the rational design and manufacture of molecular structures and dynamic devices made of DNA. As is the case for other technologies that deal with manipulation of matter, rational development requires high quality and informative feedback on the building blocks and final products. For DNA nanotechnology such feedback is typically provided by gel electrophoresis, atomic force microscopy (AFM), and transmission electron microscopy (TEM). These analytical tools provide excellent structural information; however, usually they do not provide high-resolution dynamic information. For the development of DNA-made dynamic devices such as machines, motors, robots, and computers this constitutes a major problem. Bulk-fluorescence techniques are capable of providing dynamic information, but because only ensemble averaged information is obtained, the technique may not adequately describe the dynamics in the context of complex DNA devices. The single-molecule fluorescence (SMF) technique offers a unique combination of capabilities that make it an excellent tool for guiding the development of DNA-made devices. The technique has been increasingly used in DNA nanotechnology, especially for the analysis of structure, dynamics, integrity, and operation of DNA-made devices; however, its capabilities are not yet sufficiently familiar to the community. The purpose of this Account is to demonstrate how different SMF tools can be utilized for the development of DNA devices and for structural dynamic investigation of biomolecules in general and DNA molecules in particular. Single-molecule diffusion-based Förster resonance energy transfer and alternating laser excitation (sm-FRET/ALEX) and immobilization-based total internal reflection fluorescence (TIRF) techniques are briefly described and demonstrated. To illustrate the many applications of SMF to DNA nanotechnology, examples of SMF studies of DNA hairpins and Holliday junctions and of the interactions of DNA strands with DNA origami and origami-related devices such as a DNA bipedal motor are provided. These examples demonstrate how SMF can be utilized for measurement of distances and conformational distributions and equilibrium and nonequilibrium kinetics, to monitor structural integrity and operation of DNA devices, and for isolation and investigation of minor subpopulations including malfunctioning and nonreactive devices. Utilization of a flow-cell to achieve measurements of dynamics with increased time resolution and for convenient and efficient operation of DNA devices is discussed briefly. We conclude by summarizing the various benefits provided by SMF for the development of DNA nanotechnology and suggest that the method can significantly assist in the design and manufacture and evaluation of operation of DNA devices.

Published

2014

2. Detailed Study of DNA Hairpin Dynamics Using Single-Molecule Fluorescence Assisted by DNA Origami

Author

Eyal Nir, Toma E. Tomov, Miran Liber, Hagai Drory, Roman Tsukanov, Noa Plavner, and Rula Masoud

Subjects

Chemistry, Inverted Repeat Sequences, Immobilized Nucleic Acids, Fluorescence correlation spectroscopy, DNA, Sodium Chloride, Single-molecule experiment, Fluorescence, Surfaces, Coatings and Films, Gibbs free energy, Diffusion, Crystallography, symbols.namesake, Förster resonance energy transfer, Ionic strength, Metastability, Fluorescence Resonance Energy Transfer, Materials Chemistry, symbols, Thermodynamics, DNA origami, Physical and Theoretical Chemistry

Abstract

The dynamics of two DNA hairpins (5'-TCGCCT-A31-AGGCGA-3' and 5'-TCGCCG-A31-CGGCGA-3') were studied using immobilization-based and diffusion-based single-molecule fluorescence techniques. The techniques enabled separated and detailed investigation of the states and of the transition reactions. Only two states, open and closed, were identified from analysis of the FRET histograms; metastable states with lifetimes longer than the technique resolution (0.3 ms) were not observed. The opening and closing reaction rates were determined directly from the FRET time trajectories, and the Gibbs free energies of these states and of the transition state were calculated using the Kramer theory. The rates, which are undoubtedly of transitions between the fully closed and the fully open states and ranged from 2 to 90 s(-1), were lower (∼10-fold) than the rates previously determined from fluorescence correlation spectroscopy. The heights of the barriers for closing were almost identical for the two hairpins. The barrier for opening the hairpin with the stronger stem was higher (4.3 kJ/mol) than that for the hairpin with the weaker stem, in very good agreement with the difference in stability calculated by the nearest-neighbor method. The barrier for closing the hairpin decreased (∼8 kJ/mol) and the barrier for opening increased (∼4 kJ/mol) with increasing NaCl concentration (10-100 mM), indicating that higher ionic strength stabilizes the folded state with respect to the transition state and stabilizes the transition state relative to the unfolded state. The very good agreements in the dynamics measured for free hairpins, for hairpins anchored to origami, and for hairpins anchored to the coverslip and the very good agreement between the two single-molecule techniques demonstrate that neither the origami nor the coverslip influence the hairpin dynamics, supporting a previous demonstration that origami can serve as a platform for biophysical investigations.

Published

2013

3. Studying the Structural Dynamics of Bipedal DNA Motors with Single-Molecule Fluorescence Spectroscopy

Author

Miran Liber, Eyal Nir, Rula Masoud, Noa Plavner, Roman Tsukanov, and Toma E. Tomov

Subjects

Work (thermodynamics), Chemistry, Lasers, General Engineering, Phase (waves), General Physics and Astronomy, Nanotechnology, DNA, Single-molecule experiment, Kinetics, Motion, chemistry.chemical_compound, Spectrometry, Fluorescence, Förster resonance energy transfer, Yield (chemistry), DNA nanotechnology, Fluorescence Resonance Energy Transfer, General Materials Science, Spectroscopy, Biological system, Fluorescent Dyes

Abstract

We present a test case example of a detailed single-molecule fluorescence study of one of the most sophisticated and complex DNA devices introduced to date, a recently published autonomous bipedal DNA motor. We used the diffusion-based single-molecule Förster resonance energy transfer technique, coupled to alternating laser excitation (sm-FRET-ALEX), to monitor the motor assembly and operation. The study included verification of the formation of the correct structures, and of the correct motor operation, determination of the formation and stepping reaction yields, and identification of side products. Finally, the mechanisms of the motor assembly and operation were elucidated by measuring the reaction kinetics profile of track-walker binding and of lifting of the walker's leg upon fuel addition. The profiles revealed a fast phase, in which about half of the reaction was completed, followed by a slow phase which adds somewhat to the yield, reflecting the incomplete motor assembly and operation identified in the equilibrium experiments. Although further study is needed to fully understand the reasons for the incomplete assembly and operation, this work demonstrates that single-molecule fluorescence, based on its ability to provide detailed in situ structural dynamics information, inaccessible for traditional methods, constitutes an excellent tool for chaperoning the development of DNA-based technology.

Published

2012

4. Disentangling Subpopulations in Single-Molecule FRET and ALEX Experiments with Photon Distribution Analysis

Author

Rula Masoud, Eyal Nir, Roman Tsukanov, Miran Liber, Toma E. Tomov, and Noa Plavner

Subjects

Models, Molecular, Photons, Brightness, Photon, Chemistry, Lasers, Inverted Repeat Sequences, Statistics as Topic, Kernel density estimation, Spectroscopy, Imaging, and Other Techniques, Biophysics, Analytical chemistry, DNA, Single-molecule FRET, Förster resonance energy transfer, Histogram, Fluorescence Resonance Energy Transfer, Nucleic Acid Conformation, DNA origami, A-DNA, Biological system

Abstract

Among the advantages of the single-molecule approach when used to study biomolecular structural dynamics and interaction is its ability to distinguish between and independently observe minor subpopulations. In a single-molecule Förster resonance energy transfer (FRET) and alternating laser excitation diffusion experiment, the various populations are apparent in the resultant histograms. However, because histograms are calculated based on the per-burst mean FRET and stoichiometry ratio and not on the internal photon distribution, much of the acquired information is lost, thereby reducing the capabilities of the method. Here we suggest what to our knowledge is a novel statistical analysis tool that significantly enhances these capabilities, and we use it to identify and isolate static and dynamic subpopulations. Based on a kernel density estimator and a proper photon distribution analysis, for each individual burst, we calculate scores that reflect properties of interest. Specifically, we determine the FRET efficiency and brightness ratio distributions and use them to reveal 1), the underlying structure of a two-state DNA-hairpin and a DNA hairpin that is bound to DNA origami; 2), a minor doubly labeled dsDNA subpopulation concealed in a larger singly labeled dsDNA; and 3), functioning DNA origami motors concealed within a larger subpopulation of defective motors. Altogether, these findings demonstrate the usefulness of the proposed approach. The method was developed and tested using simulations, its rationality is described, and a computer algorithm is provided.

Published

2012

5. Nucleosome Core Particle Disassembly and Assembly Kinetics Studied Using Single-Molecule Fluorescence

Author

Yaron Berger, Eyal Nir, Toma E. Tomov, Noa Plavner Hazan, Katalin Tóth, Roman Tsukanov, Joerg Langowski, Rula Masoud, and Miran Liber

Subjects

biology, Chemistry, Kinetics, Biophysics, Sodium Chloride, Single-molecule experiment, Dissociation (chemistry), Fluorescence, Nucleosomes, Crystallography, chemistry.chemical_compound, Xenopus laevis, Histone, Förster resonance energy transfer, biology.protein, Escherichia coli, Fluorescence Resonance Energy Transfer, Nucleosome, Animals, Proteins and Nucleic Acids, Dimerization, DNA, Macromolecule

Abstract

The stability of the nucleosome core particle (NCP) is believed to play a major role in regulation of gene expression. To understand the mechanisms that influence NCP stability, we studied stability and dissociation and association kinetics under different histone protein (NCP) and NaCl concentrations using single-pair Förster resonance energy transfer and alternating laser excitation techniques. The method enables distinction between folded, unfolded, and intermediate NCP states and enables measurements at picomolar to nanomolar NCP concentrations where dissociation and association reactions can be directly observed. We reproduced the previously observed nonmonotonic dependence of NCP stability on NaCl concentration, and we suggest that this rather unexpected behavior is a result of interplay between repulsive and attractive forces within positively charged histones and between the histones and the negatively charged DNA. Higher NaCl concentrations decrease the attractive force between the histone proteins and the DNA but also stabilize H2A/H2B histone dimers, and possibly (H3/H4)2 tetramers. An intermediate state in which one DNA arm is unwrapped, previously observed at high NaCl concentrations, is also explained by this salt-induced stabilization. The strong dependence of NCP stability on ion and histone concentrations, and possibly on other charged macromolecules, may play a role in chromosomal morphology.

Published

2015

6. Conformational dynamics of DNA hairpins at millisecond resolution obtained from analysis of single-molecule FRET histograms

Author

Yaron Berger, Eyal Nir, Roman Tsukanov, Toma E. Tomov, and Miran Liber

Subjects

Total internal reflection fluorescence microscope, Base Sequence, Resolution (electron density), Single-molecule FRET, DNA, Surfaces, Coatings and Films, Folding (chemistry), Crystallography, Transition state theory, chemistry.chemical_compound, Förster resonance energy transfer, chemistry, Materials Chemistry, Biophysics, Fluorescence Resonance Energy Transfer, DNA origami, Nucleic Acid Conformation, Physical and Theoretical Chemistry

Abstract

Here we provide high resolution study of DNA hairpin dynamics achieved by probability distribution analysis (PDA) of diffusion-based single-molecule Förster resonance energy transfer (sm-FRET) histograms. The opening and closing rates of three hairpins both free and attached to DNA origami were determined. The agreement with rates previously obtained using the total internal reflection (TIRF) technique and between free hairpins and hairpins attached to origami validated the PDA and demonstrated that the origami had no influence on the hairpin dynamics. From comparison of rates of four DNA hairpins, differing only in stem sequence, and from comparison with rates calculated using nearest-neighbor method and standard transition state theory, we conclude that the unfolding reaction resembles that of melting of DNA duplex with a corresponding sequence and that the folding reaction depends on counterion concentration and not on stem sequence. Our validation and demonstration of the PDA method will encourage its implementation in future high-resolution dynamic studies of freely diffusing biomolecules.

Published

2013