118 research outputs found
Quantum Interference of Tunably Indistinguishable Photons from Remote Organic Molecules
We demonstrate two-photon interference using two remote single molecules as
bright solid-state sources of indistinguishable photons. By varying the
transition frequency and spectral width of one molecule, we tune and explore
the effect of photon distinguishability. We discuss future improvements on the
brightness of single-photon beams, their integration by large numbers on chips,
and the extension of our experimental scheme to coupling and entanglement of
distant molecules
Water Dynamics at Protein Interfaces: Ultrafast Optical Kerr Effect Study
The behavior of water molecules surrounding a protein can have an important bearing on its structure and function. Consequently, a great deal of attention has been focused on changes in the relaxation dynamics of water when it is located at the protein surface. Here we use the ultrafast optical Kerr effect to study the H-bond structure and dynamics of aqueous solutions of proteins. Measurements are made for three proteins as a function of concentration. We find that the water dynamics in the first solvation layer of the proteins are slowed by up to a factor of 8 in comparison to those in bulk water. The most marked slowdown was observed for the most hydrophilic protein studied, bovine serum albumin, whereas the most hydrophobic protein, trypsin, had a slightly smaller effect. The terahertz Raman spectra of these protein solutions resemble those of pure water up to 5 wt % of protein, above which a new feature appears at 80 cm–1, which is assigned to a bending of the protein amide chain
Influence of supramolecular forces on the linear viscoelasticity of gluten
Stress relaxation behavior of hydrated gluten networks was investigated by means of rheometry combined with μ-computed tomography (μ-CT) imaging. Stress relaxation behavior was followed over a wide temperature range (0–70 °C). Modulation of intermolecular bonds was achieved with urea or ascorbic acid in an effort to elucidate the presiding intermolecular interactions over gluten network relaxation. Master curves of viscoelasticity were constructed, and relaxation spectra were computed revealing three relaxation regimes for all samples. Relaxation commences with a well-defined short-time regime where Rouse-like modes dominate, followed by a power law region displaying continuous relaxation concluding in a terminal zone. In the latter zone, poroelastic relaxation due to water migration in the nanoporous structure of the network also contributes to the stress relief in the material. Hydrogen bonding between adjacent protein chains was identified as the determinant force that influences the relaxation of the networks. Changes in intermolecular interactions also resulted in changes in microstructure of the material that was also linked to the relaxation behavior of the networks
Disaccharide topology induces slow down in local water dynamics
Molecular level insight into water structure and structural dynamics near proteins, lipids and
nucleic acids is critical to the quantitative understanding of many biophysical processes. Un-
fortunately, understanding hydration and hydration dynamics around such large molecules is challenging because of the necessity of deconvoluting the effects of topography and chemical heterogeneity. Here we study, via classical all atom simulation, water structure and structural dynamics around two biologically relevant solutes large enough to have significant chemical and topological heterogeneity but small enough to be computationally tractable: the disaccharides Kojibiose and Trehalose. We find both molecules to be strongly amphiphilic (as quantified from normalized local density fluctuations) and to induce nonuniform local slowdown in water translational and rotational motion. Detailed analysis of the rotational slowdown shows that while the rotational mechanism is similar to that previously identified in other aqueous systems by Laage, Hynes and coworkers, two novel characteristics are observed: broadening of the transition state during hydrogen bond exchange (water rotation) and a subpopulation of water for which rotation is slowed because of hindered access of the new accepting water molecule to the transition state. Both of these characteristics are expected to be generic features of water rotation around larger biomolecules and, taken together, emphasize the difficulty in transferring insight into water rotation around small molecules to much larger amphiphilic
solutes.This work is part of the research program of the “Stichting voor Fundamenteel Onderzoek der
Materie (FOM)” which is financially supported by the “Nederlandse organisatie voor Wetenschap-
pelijk Onderzoek (NWO)”. Further financial support was provided by a Marie Curie Incoming
International Fellowship (RKC). We gratefully acknowledge SARA, the Dutch center for high-
performance computing, for computational time and Huib Bakker and Daan Frenkel for useful
critical reviews on an earlier version of this work. We thank two anonymous reviewers for their
excellent work, especially for bringing to our attention calculations done on the transition state geometry of dimers and the overstructuring of the O-O radial distribution function of SPC/E water
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Temperature dependence of protein dynamics simulated with three different water models
The effect of variation of the water model on the temperature dependence of protein and hydration water dynamics is examined by performing molecular dynamics simulations of myoglobin with the TIP3P, TIP4P, and TIP5P water models and the CHARMM protein force field at temperatures between 20 and 300 K. The atomic mean-square displacements, solvent reorientational relaxation times, pair angular correlations between surface water molecules, and time-averaged structures of the protein are all found to be similar, and the protein dynamical transition is described almost indistinguishably for the three water potentials. The results provide evidence that for some purposes changing the water model in protein simulations without a loss of accuracy may be possible
Photon-Atom Coupling with Parabolic Mirrors
Efficient coupling of light to single atomic systems has gained considerable
attention over the past decades. This development is driven by the continuous
growth of quantum technologies. The efficient coupling of light and matter is
an enabling technology for quantum information processing and quantum
communication. And indeed, in recent years much progress has been made in this
direction. But applications aside, the interaction of photons and atoms is a
fundamental physics problem. There are various possibilities for making this
interaction more efficient, among them the apparently 'natural' attempt of
mode-matching the light field to the free-space emission pattern of the atomic
system of interest. Here we will describe the necessary steps of implementing
this mode-matching with the ultimate aim of reaching unit coupling efficiency.
We describe the use of deep parabolic mirrors as the central optical element of
a free-space coupling scheme, covering the preparation of suitable modes of the
field incident onto these mirrors as well as the location of an atom at the
mirror's focus. Furthermore, we establish a robust method for determining the
efficiency of the photon-atom coupling.Comment: Book chapter in compilation "Engineering the Atom-Photon Interaction"
published by Springer in 2015, edited by A. Predojevic and M. W. Mitchell,
ISBN 9783319192307, http://www.springer.com/gp/book/9783319192307. Only
change to version1: now with hyperlinks to arXiv eprints of other book
chapters mentioned in this on
Predictors of disease worsening defined by progression of organ damage in diffuse systemic sclerosis: a European Scleroderma Trials and Research (EUSTAR) analysis.
Objectives Mortality and worsening of organ function are desirable endpoints for clinical trials in systemic sclerosis (SSc). The aim of this study was to identify factors that allow enrichment of patients with these endpoints, in a population of patients from the European Scleroderma Trials and Research group database. Methods Inclusion criteria were diagnosis of diffuse SSc and follow-up over 12\ub13 months. Disease worsening/organ progression was fulfilled if any of the following events occurred: new renal crisis; decrease of lung or heart function; new echocardiography-suspected pulmonary hypertension or death. In total, 42 clinical parameters were chosen as predictors for the analysis by using (1) imputation of missing data on the basis of multivariate imputation and (2) least absolute shrinkage and selection operator regression. Results Of 1451 patients meeting the inclusion criteria, 706 had complete data on outcome parameters and were included in the analysis. Of the 42 outcome predictors, eight remained in the final regression model. There was substantial evidence for a strong association between disease progression and age, active digital ulcer (DU), lung fibrosis, muscle weakness and elevated C-reactive protein (CRP) level. Active DU, CRP elevation, lung fibrosis and muscle weakness were also associated with a significantly shorter time to disease progression. A bootstrap validation step with 10 000 repetitions successfully validated the model. Conclusions The use of the predictive factors presented here could enable cohort enrichment with patients at risk for overall disease worsening in SSc clinical trial
Effect of urea on the structural dynamics of water
We use polarization-resolved mid-infrared pump-probe spectroscopy to study the effect of urea on the structure and dynamics of water. Surprisingly, we find that, even at high concentrations of urea (8 M), the orientational dynamics of most water molecules are the same as in pure liquid water, showing that urea has a negligible effect on the hydrogen-bond dynamics of these molecules. However, a small fraction of the water molecules (approximately one water molecule per urea molecule) turns out to be strongly immobilized by urea, displaying orientational dynamics that are more than six times slower than in bulk water. A likely explanation is that these water molecules are tightly associated with urea, forming specific urea–water complexes. We discuss these results in light of the protein denaturing ability of aqueous urea
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