5,482 research outputs found
Single-copy entanglement in a gapped quantum spin chain
The single-copy entanglement of a given many-body system is defined [J.
Eisert and M. Cramer, Phys. Rev. A. 72, 042112 (2005)] as the maximal
entanglement deterministically distillable from a bipartition of a single
specimen of that system. For critical (gapless) spin chains, it was recently
shown that this is exactly half the von Neumann entropy [R. Orus, J. I.
Latorre, J. Eisert, and M. Cramer, Phys. Rev. A 73, 060303(R) (2006)], itself
defined as the entanglement distillable in the asymptotic limit: i.e. given an
infinite number of copies of the system. It is an open question as to what the
equivalent behaviour for gapped systems is. In this paper, I show that for the
paradigmatic spin-S Affleck-Kennedy-Lieb-Tasaki chain (the archetypal gapped
chain), the single-copy entanglement is equal to the von Neumann entropy: i.e.
all the entanglement present may be distilled from a single specimen.Comment: Typos corrected; accepted for publication in Phys. Rev. Lett.;
comments welcom
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Interleukin-2 druggability is modulated by global conformational transitions controlled by a helical capping switch.
Interleukin-2 (IL-2) is a small α-helical cytokine that regulates immune cell homeostasis through its recruitment to a high-affinity heterotrimeric receptor complex (IL-2Rα/IL-2Rβ/γc). IL-2 has been shown to have therapeutic efficacy for immune diseases by preferentially expanding distinct T cell compartments, and several regulatory T cell (Treg)-biasing anti-IL-2 antibodies have been developed for combination therapies. The conformational plasticity of IL-2 plays an important role in its biological actions by modulating the strength of receptor and drug interactions. Through an NMR analysis of milliseconds-timescale dynamics of free mouse IL-2 (mIL-2), we identify a global transition to a sparse conformation which is regulated by an α-helical capping "switch" at the loop between the A and B helices (AB loop). Binding to either an anti-mouse IL-2 monoclonal antibody (mAb) or a small molecule inhibitor near the loop induces a measurable response at the core of the structure, while locking the switch to a single conformation through a designed point mutation leads to a global quenching of core dynamics accompanied by a pronounced effect in mAb binding. By elucidating key details of the long-range allosteric communication between the receptor binding surfaces and the core of the IL-2 structure, our results offer a direct blueprint for designing precision therapeutics targeting a continuum of conformational states
Irradiation of an Accretion Disc by a Jet: General Properties and Implications for Spin Measurements of Black Holes
X-ray irradiation of the accretion disc leads to strong reflection features,
which are then broadened and distorted by relativistic effects. We present a
detailed, general relativistic approach to model this irradiation for different
geometries of the primary X-ray source. These geometries include the standard
point source on the rotational axis as well as more jet-like sources, which are
radially elongated and accelerating. Incorporating this code in the relline
model for relativistic line emission, the line shape for any configuration can
be predicted. We study how different irradiation geometries affect the
determination of the spin of the black hole. Broad emission lines are produced
only for compact irradiating sources situated close to the black hole. This is
the only case where the black hole spin can be unambiguously determined. In all
other cases the line shape is narrower, which could either be explained by a
low spin or an elongated source. We conclude that for all those cases and
independent of the quality of the data, no unique solution for the spin exists
and therefore only a lower limit of the spin value can be given.Comment: accepted by MNRAS for publication; now proof corrected Versio
The importance of the lipoxygenase-hepoxilin pathway in the mammalian epidermal barrier
This review covers the background to discovery of the two key lipoxygenases (LOX) involved in epidermal barrier function, 12R-LOX and eLOX3, and our current views on their functioning. In the outer epidermis, their consecutive actions oxidize linoleic acid esterified in ω-hydroxy-ceramide to a hepoxilin-related derivative. The relevant background to hepoxilin and trioxilin biochemistry is briefly reviewed. We outline the evidence that linoleate in the ceramide is the natural substrate of the two LOX enzymes and our proposal for its importance in construction of the epidermal water barrier. Our hypothesis is that the oxidation promotes hydrolysis of the oxidized linoleate moiety from the ceramide. The resulting free ω-hydroxyl of the ω-hydroxyceramide is covalently bound to proteins on the surface of the corneocytes to form the corneocyte lipid envelope, a key barrier component. Understanding the role of the LOX enzymes and their hepoxilin products should provide rational approaches to ameliorative therapy for a number of the congenital ichthyoses involving compromised barrier function. This article is part of a Special Issue entitled The Important Role of Lipids in the Epidermis and their Role in the Formation and Maintenance of the Cutaneous Barrier. Guest Editors: Kenneth R. Feingold and Peter Elias
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Predicting Progression in Parkinson's Disease Using Baseline and 1-Year Change Measures.
BackgroundImproved prediction of Parkinson's disease (PD) progression is needed to support clinical decision-making and to accelerate research trials.ObjectivesTo examine whether baseline measures and their 1-year change predict longer-term progression in early PD.MethodsParkinson's Progression Markers Initiative study data were used. Participants had disease duration ≤2 years, abnormal dopamine transporter (DAT) imaging, and were untreated with PD medications. Baseline and 1-year change in clinical, cerebrospinal fluid (CSF), and imaging measures were evaluated as candidate predictors of longer-term (up to 5 years) change in Movement Disorders Society-Unified Parkinson's Disease Rating Scale (MDS-UPDRS) score and DAT specific binding ratios (SBR) using linear mixed-effects models.ResultsAmong 413 PD participants, median follow-up was 5 years. Change in MDS-UPDRS from year-2 to last follow-up was associated with disease duration (β= 0.351; 95% CI = 0.146, 0.555), male gender (β= 3.090; 95% CI = 0.310, 5.869), and baseline (β= -0.199; 95% CI = -0.315, -0.082) and 1-year change (β= 0.540; 95% CI = 0.423, 0.658) in MDS-UPDRS; predictors in the model accounted for 17.6% of the variance in outcome. Predictors of percent change in mean SBR from year-2 to last follow-up included baseline rapid eye movement sleep behavior disorder score (β= -0.6229; 95% CI = -1.2910, 0.0452), baseline (β= 7.232; 95% CI = 2.268, 12.195) and 1-year change (β= 45.918; 95% CI = 35.994,55.843) in mean striatum SBR, and 1-year change in autonomic symptom score (β= -0.325;95% CI = -0.695, 0.045); predictors in the model accounted for 44.1% of the variance.ConclusionsBaseline clinical, CSF, and imaging measures in early PD predicted change in MDS-UPDRS and dopamine-transporter binding, but the predictive value of the models was low. Adding the short-term change of possible predictors improved the predictive value, especially for modeling change in dopamine-transporter binding
Molecular beam growth of graphene nanocrystals on dielectric substrates
We demonstrate the growth of graphene nanocrystals by molecular beam methods
that employ a solid carbon source, and that can be used on a diverse class of
large area dielectric substrates. Characterization by Raman and Near Edge X-ray
Absorption Fine Structure spectroscopies reveal a sp2 hybridized hexagonal
carbon lattice in the nanocrystals. Lower growth rates favor the formation of
higher quality, larger size multi-layer graphene crystallites on all
investigated substrates. The surface morphology is determined by the roughness
of the underlying substrate and graphitic monolayer steps are observed by
ambient scanning tunneling microscopy.Comment: Accepted in Carbon; Discussion section added; 20 pages, 6 figures (1
updated
Studies of Minerals, Organic and Biogenic Materials through Time-Resolved Raman Spectroscopy
A compact remote Raman spectroscopy system was developed at NASA Langley Research center and was previously demonstrated for its ability to identify chemical composition of various rocks and minerals. In this study, the Raman sensor was utilized to perform time-resolved Raman studies of various samples such as minerals and rocks, Azalea leaves and a few fossil samples. The Raman sensor utilizes a pulsed 532 nm Nd:YAG laser as excitation source, a 4-inch telescope to collect the Raman-scattered signal from a sample several meters away, a spectrograph equipped with a holographic grating, and a gated intensified CCD (ICCD) camera system. Time resolved Raman measurements were carried out by varying the gate delay with fixed short gate width of the ICCD camera, allowing measurement of both Raman signals and fluorescence signals. Rocks and mineral samples were characterized including marble, which contain CaCO3. Analysis of the results reveals the short (approx.10-13 s) lifetime of the Raman process, and shows that Raman spectra of some mineral samples contain fluorescence emission due to organic impurities. Also analyzed were a green (pristine) and a yellow (decayed) sample of Gardenia leaves. It was observed that the fluorescence signals from the green and yellow leaf samples showed stronger signals compared to the Raman lines. Moreover, it was also observed that the fluorescence of the green leaf was more intense and had a shorter lifetime than that of the yellow leaf. For the fossil samples, Raman shifted lines could not be observed due the presence of very strong short-lived fluorescence
Design and Build a Compact Raman Sensor for Identification of Chemical Composition
A compact remote Raman sensor system was developed at NASA Langley Research Center. This sensor is an improvement over the previously reported system, which consisted of a 532 nm pulsed laser, a 4-inch telescope, a spectrograph, and an intensified charge-coupled devices (CCD) camera. One of the attractive features of the previous system was its portability, thereby making it suitable for applications such as planetary surface explorations, homeland security and defense applications where a compact portable instrument is important. The new system was made more compact by replacing bulky components with smaller and lighter components. The new compact system uses a smaller spectrograph measuring 9 x 4 x 4 in. and a smaller intensified CCD camera measuring 5 in. long and 2 in. in diameter. The previous system was used to obtain the Raman spectra of several materials that are important to defense and security applications. Furthermore, the new compact Raman sensor system is used to obtain the Raman spectra of a diverse set of materials to demonstrate the sensor system's potential use in the identification of unknown materials
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