783 research outputs found
Spin- and time-resolved photoemission studies of thin Co2FeSi Heusler alloy films
We have studied the possibly half metallic Co2FeSi full Heusler alloy by
means of spin- and time-resolved photoemission spectroscopy. For excitation,
the second and fourth harmonic of femtosecond Ti:sapphire lasers were used,
with photon energies of 3.1 eV and 5.9 eV, respectively. We compare the
dependence of the measured surface spin polarization on the particular
photoemission mechanism, i.e. 1-photon-photoemission (1PPE) or 2-photon
photoemission (2PPE). The observed differences in the spin polarization can be
explained by a spin-dependent lifetime effect occurring in the 2-photon
absorption process. The difference in escape depth of the two methods in this
context suggests that the observed reduction of spin polarization (compared to
the bulk) cannot be attributed just to the outermost surface layer but takes
place at least 4-6 nm away from the surface.Comment: 7 pages, 3 figures; submitted to Journal of Magnetism and Magnetic
Material
Direct evidence for efficient ultrafast charge separation in epitaxial WS/graphene heterostructure
We use time- and angle-resolved photoemission spectroscopy (tr-ARPES) to
investigate ultrafast charge transfer in an epitaxial heterostructure made of
monolayer WS and graphene. This heterostructure combines the benefits of a
direct gap semiconductor with strong spin-orbit coupling and strong
light-matter interaction with those of a semimetal hosting massless carriers
with extremely high mobility and long spin lifetimes. We find that, after
photoexcitation at resonance to the A-exciton in WS, the photoexcited holes
rapidly transfer into the graphene layer while the photoexcited electrons
remain in the WS layer. The resulting charge transfer state is found to
have a lifetime of \,ps. We attribute our findings to differences in
scattering phase space caused by the relative alignment of WS and graphene
bands as revealed by high resolution ARPES. In combination with spin-selective
excitation using circularly polarized light the investigated WS/graphene
heterostructure might provide a new platform for efficient optical spin
injection into graphene.Comment: 28 pages, 14 figure
Direct evidence for efficient ultrafast charge separation in epitaxial WS<sub>2</sub>/graphene heterostructures
We use time- and angle-resolved photoemission spectroscopy (tr-ARPES) to investigate ultrafast charge transfer in an epitaxial heterostructure made of monolayer WS2 and graphene. This heterostructure combines the benefits of a direct-gap semiconductor with strong spin-orbit coupling and strong light-matter interaction with those of a semimetal hosting massless carriers with extremely high mobility and long spin lifetimes. We find that, after photoexcitation at resonance to the A-exciton in WS2, the photoexcited holes rapidly transfer into the graphene layer while the photoexcited electrons remain in the WS2 layer. The resulting charge-separated transient state is found to have a lifetime of ∼1 ps. We attribute our findings to differences in scattering phase space caused by the relative alignment of WS2 and graphene bands as revealed by high-resolution ARPES. In combination with spin-selective optical excitation, the investigated WS2/graphene heterostructure might provide a platform for efficient optical spin injection into graphene
Anti-transglutaminase 6 antibodies in children and young adults with cerebral palsy.
Objectives. We have previously reported a high prevalence of gluten-related serological markers (GRSM) in children and young adults with cerebral palsy (CP). The majority had no enteropathy to suggest coeliac disease (CD). Antibodies against transglutaminase 6 (anti-TG6) represent a new marker associated with gluten-related neurological dysfunction. The aim of this study was to investigate the prevalence of anti-TG6 antibodies in this group of individuals with an early neurological injury resulting in CP. Materials and Methods. Sera from 96 patients with CP and 36 controls were analysed for IgA/IgG class anti-TG6 by ELISA. Results. Anti-TG6 antibodies were found in 12/96 (13%) of patients with CP compared to 2/36 (6%) in controls. The tetraplegic subgroup of CP had a significantly higher prevalence of anti-TG6 antibodies 6/17 (35%) compared to the other subgroups and controls. There was no correlation of anti-TG6 autoantibodies with seropositivity to food proteins including gliadin. Conclusions. An early brain insult and associated inflammation may predispose to future development of TG6 autoimmunity
Quantum-Well Wavefunction Localization and the Electron-Phonon Interaction in Thin Ag Nanofilms
The electron-phonon interaction in thin Ag-nanofilms epitaxially grown on
Cu(111) is investigated by temperature-dependent and angle-resolved
photoemission from silver quantum-well states. Clear oscillations in the
electron-phonon coupling parameter as a function of the silver film thickness
are observed. Different from other thin film systems where quantum oscillations
are related to the Fermi-level crossing of quantum-well states, we can identify
a new mechanism behind these oscillations, based on the wavefunction
localization of the quantum-well states in the film
TG6 auto-antibodies in dermatitis herpetiformis
Dermatitis herpetiformis (DH) is an extraintestinal manifestation of gluten sensitivity, in which an autoimmune response is directed against transglutaminase 3 (TG3), an epidermal transglutaminase. TG2 is the autoantigen in celiac disease (CD), defined by the presence of enteropathy, and TG6 is the autoantigen in neurological manifestations of gluten sensitivity. The interplay between B cell responses to these 3 transglutaminases in developing the clinical spectrum of disease manifestations is not completely understood. Also, the individual or combined diagnostic and predictive value of the respective autoantibodies is not fully explored. We examined the prevalence of TG6 antibodies in a cohort of patients with DH. TG6 positivity was found in 13/33 (39%), with IgA detected in 11 patients, IgG in 3, and both in 1. This was significantly higher compared to what is seen in the classic CD cases (14%) in a Finnish population. TG6 positive baseline samples constituted 60% of DH patients with no enteropathy (n = 10), as opposed to 17% positivity in those with overt enteropathy (n = 12; Marsh IIIB). Repeat testing after adherence to a gluten-free diet for 1 year showed reduced titers for TG6 antibodies in 11/13 (85%), whereby 7 patients were now TG6 antibody-negative. Four patients seroconverted and tested positive for TG6 antibodies at one year, due to the ongoing exposure to gluten. We report another patient who presented with neurological manifestations (encephalopathy) leading to the diagnosis of CD, who was intermittently adhering to a gluten-free diet. Serological testing at baseline showed him to be positive for antibodies to all 3 transglutaminases. Eleven years later, he developed DH. He also subsequently developed ataxia and peripheral neuropathy. Although TG3 and TG6 autoantibodies are linked to certain disease manifestations, TG2, TG3, and TG6 autoantibodies can be present across the spectrum of GRD patients and might develop years before onset of symptoms of extraintestinal manifestations. This is consistent with gluten-dependent adaptive immunity being a necessary but not sufficient pretext to organ-specific damage. TG6 antibodies appear to develop more frequently in patients where tolerance to gluten was broken but, either there was no development of the molecular state driving the tissue destruction at the level of the gut, or perhaps more likely, there was more resistance to developing this phenotype
Cell surface localization of tissue transglutaminase is dependent on a fibronectin-binding site in its N-terminal beta-sandwich domain
Increasing evidence indicates that tissue transglutaminase (tTG) plays a role in the assembly and remodeling of extracellular matrices and promotes cell adhesion. Using an inducible system we have previously shown that tTG associates with the extracellular matrix deposited by stably transfected 3T3 fibroblasts overexpressing the enzyme. We now show by confocal microscopy that tTG colocalizes with pericellular fibronectin in these cells, and by immunogold electron microscopy that the two proteins are found in clusters at the cell surface. Expression vectors encoding the full-length tTG or a N-terminal truncated tTG lacking the proposed fibronectin-binding site (fused to the bacterial reporter enzyme β-galactosidase) were generated to characterize the role of fibronectin in sequestration of tTG in the pericellular matrix. Enzyme-linked immunosorbent assay style procedures using extracts of transiently transfected COS-7 cells and immobilized fibronectin showed that the truncation abolished fibronectin binding. Similarly, the association of tTG with the pericellular matrix of cells in suspension or with the extracellular matrix deposited by cell monolayers was prevented by the truncation. These results demonstrate that tTG binds to the pericellular fibronectin coat of cells via its N-terminal β-sandwich domain and that this interaction is crucial for cell surface association of tTG
Experimental time-resolved photoemission and ab initio study of lifetimes of excited electrons in Mo and Rh
We have studied the relaxation dynamics of optically excited electrons in
molybdenum and rhodium by means of time resolved two-photon photoemission
spectroscopy (TR-2PPE) and ab initio electron self-energy calculations
performed within the GW and GW+T approximations. Both theoretical approaches
reproduce qualitatively the experimentally observed trends and differences in
the lifetimes of excited electrons in molybdenum and rhodium. For excitation
energies exceeding the Fermi energy by more than 1 eV, the GW+T theory yields
lifetimes in quantitative agreement with the experimental results. As one of
the relevant mechanisms causing different excited state lifetime in Mo and Rh
we identify the occupation of the 4d bands. An increasing occupation of the 4d
bands results in an efficient decrease of the lifetime even for rather small
excitation energies of a few 100 meV.Comment: 8 pages, 10 figure
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