88 research outputs found
Thin Film, Near-Surface and Multi-Layer Investigations by Low-Energy μ +SR
At the Paul Scherrer Institute (PSI, Villigen, Switzerland) the beam of low-energy positive polarised muons (LE-μ +) with tunable energy between 0.5 and 30keV allows the extension of the muon-spin-rotation technique (μSR) to studies on thin films and multi-layers (LE-μ +SR). The range of these muons in solids covers the near-surface region up to implantation depths of about 300nm. As a sensitive local magnetic probe with a complementary observational time window to other techniques LE-μ +SR offers the unique possibility to gain new insights in these nano-scale objects. After outlining the current status of the LE-μ + beam line we demonstrate the potential of this new technique by presenting the results of recent experiments: i) the direct observation of non-local effects in a superconducting Pb film, ii) the oxygen isotope effect on the in-plane penetration depth in optimally doped , and iii) the first observation of the conduction electron spin polarisation in the Ag spacer of a Fe/Ag/Fe tri-laye
Weak ferromagnetism with very large canting in a chiral lattice: (pyrimidine)2FeCl2
The transition metal coordination compound (pyrimidine)2FeCl2 crystallizes in
a chiral lattice, space group I 4_1 2 2 (or I4_3 2 2). Combined magnetization,
Mossbauer spectroscopy and powder neutron diffraction studies reveal that it is
a canted antiferromagnet below T_N = 6.4 K with an unusually large canting of
the magnetic moments of 14 deg. from their general antiferromagnetic alignment,
one of the largest reported to date. This results in weak ferromagnetism with a
ferromagnetic component of 1 mu_B. The large canting is due to the interplay
between the antiferromagnetic exchange interaction and the local single-ion
anisotropy in the chiral lattice. The magnetically ordered structure of
(pyrimidine)2FeCl2, however, is not chiral. The implications of these findings
for the search of molecule based materials exhibiting chiral magnetic ordering
is discussed.Comment: 6 pages, 5 figure
Electronic properties of LaOFFeAs in the normal state probed by NMR/NQR
We report 139La, 57Fe and 75As nuclear magnetic resonance (NMR) and nuclear
quadrupole resonance (NQR) measurements on powders of the new LaO1-xFxFeAs
superconductor for x = 0 and x = 0.1 at temperatures up to 480 K, and compare
our measured NQR spectra with local density approximation (LDA) calculations.
For all three nuclei in the x = 0.1 material, it is found that the local Knight
shift increases monotonically with an increase in temperature, and scales with
the macroscopic susceptibility, suggesting a single magnetic degree of freedom.
Surprisingly, the spin lattice relaxation rates for all nuclei also scale with
one another, despite the fact that the form factors for each site sample
different regions of q-space. This result suggests a lack of any q-space
structure in the dynamical spin susceptibility that might be expected in the
presence of antiferromagnetic correlations. Rather, our results are more
compatible with simple quasi-particle scattering. Furthermore, we find that the
increase in the electric field gradient at the As cannot be accounted for by
LDA calculations, suggesting that structural changes, in particular the
position of the As in the unit cell, dominate the NQR response.Comment: 17 pages, 6 figure
Coexistence of the spin-density-wave and superconductivity in the (Ba,K)Fe2As2
The relation between the spin-density-wave (SDW) and superconducting order is
a central topic in current research on the FeAs-based high Tc superconductors.
Conflicting results exist in the LaFeAs(O,F)-class of materials, for which
whether the SDW and superconductivity are mutually exclusive or they can
coexist has not been settled. Here we show that for the (Ba,K)Fe2As2 system,
the SDW and superconductivity can coexist in an extended range of compositions.
The availability of single crystalline samples and high value of the energy
gaps would make the materials a model system to investigate the high Tc
ferropnictide superconductivity.Comment: 4 pages, 5 figure
An extracellular steric seeding mechanism for Eph-ephrin signaling platform assembly
Erythropoetin-producing hepatoma (Eph) receptors are cell-surface protein tyrosine kinases mediating cell-cell communication. Upon activation, they form signaling clusters. We report crystal structures of the full ectodomain of human EphA2 (eEphA2) both alone and in complex with the receptor-binding domain of the ligand ephrinA5 (ephrinA5 RBD). Unliganded eEphA2 forms linear arrays of staggered parallel receptors involving two patches of residues conserved across A-class Ephs. eEphA2-ephrinA5 RBD forms a more elaborate assembly, whose interfaces include the same conserved regions on eEphA2, but rearranged to accommodate ephrinA5 RBD. Cell-surface expression of mutant EphA2s showed that these interfaces are critical for localization at cell-cell contacts and activation-dependent degradation. Our results suggest a 'nucleation' mechanism whereby a limited number of ligand-receptor interactions 'seed' an arrangement of receptors which can propagate into extended signaling arrays
Enhancement of the activity of phenoxodiol by cisplatin in prostate cancer cells
Phenoxodiol is a novel isoflav-3-ene, currently undergoing clinical trials, that has a broad in vitro activity against a number of human cancer cell lines. Phenoxodiol alone inhibited DU145 and PC3 in a dose- and time-dependent manner with IC50 values of 8±1 and 38±9 μM, respectively. The combination of phenoxodiol and cisplatin was synergistic in DU145, and additive in PC3, as assessed by the Chou–Talalay method. Carboplatin was also synergistic in combination with phenoxodiol in DU145 cells. The activity of the phenoxodiol and cisplatin combination was confirmed in vivo using a DU145 xenograft model in nude mice. Pharmacokinetic data from these mice suggest that the mechanism of synergy may occur through a pharmacodynamic mechanism. An intracellular cisplatin accumulation assay showed a 35% (P<0.05) increase in the uptake of cisplatin when it was combined in a ratio of 1 μM: 5 μM phenoxodiol, resulting in a 300% (P<0.05) increase in DNA adducts. Taken together, our results suggest that phenoxodiol has interesting properties that make combination therapy with cisplatin or carboplatin appealing
The structure and function of Alzheimer's gamma secretase enzyme complex
The production and accumulation of the beta amyloid protein (Aβ) is a key event in the cascade of oxidative and inflammatory processes that characterizes Alzheimer’s disease (AD). A multi-subunit enzyme complex, referred to as gamma (γ) secretase, plays a pivotal role in the generation of Aβ from its parent molecule, the amyloid precursor protein (APP). Four core components (presenilin, nicastrin, aph-1, and pen-2) interact in a high-molecular-weight complex to perform intramembrane proteolysis on a number of membrane-bound proteins, including APP and Notch. Inhibitors and modulators of this enzyme have been assessed for their therapeutic benefit in AD. However, although these agents reduce Aβ levels, the majority have been shown to have severe side effects in pre-clinical animal studies, most likely due to the enzymes role in processing other proteins involved in normal cellular function. Current research is directed at understanding this enzyme and, in particular, at elucidating the roles that each of the core proteins plays in its function. In addition, a number of interacting proteins that are not components of γ-secretase also appear to play important roles in modulating enzyme activity. This review will discuss the structural and functional complexity of the γ-secretase enzyme and the effects of inhibiting its activity
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