141 research outputs found
Domain wall structure in magnetic bilayers with perpendicular anisotropy
We study the magnetic domain wall structure in magnetic bilayers (two
ultrathin ferromagnetic layers separated by a non magnetic spacer) with
perpendicular magnetization. Combining magnetic force and ballistic electron
emission microscopies, we are able to reveal the details of the magnetic
structure of the wall with a high spatial accuracy. In these layers, we show
that the classical Bloch wall observed in single layers transforms into
superposed N\'eel walls due to the magnetic coupling between the ferromagnetic
layers. Quantitative agreement with micromagnetic calculations is achieved.Comment: Author adresses AB, SR, JM and AT: Laboratoire de Physique des
Solides, CNRS, Universit\'e Paris Sud, UMR 8502, 91405 Orsay Cedex, France ML
: Laboratoire PMTM, Institut Galil\'ee, CNRS, Universit\'e Paris-13, UPR
9001, 93430 Villetaneuse, Franc
Nanoscale magnetic field mapping with a single spin scanning probe magnetometer
We demonstrate quantitative magnetic field mapping with nanoscale resolution,
by applying a lock-in technique on the electron spin resonance frequency of a
single nitrogen-vacancy defect placed at the apex of an atomic force microscope
tip. In addition, we report an all-optical magnetic imaging technique which is
sensitive to large off-axis magnetic fields, thus extending the operation range
of diamond-based magnetometry. Both techniques are illustrated by using a
magnetic hard disk as a test sample. Owing to the non-perturbing and
quantitative nature of the magnetic probe, this work should open up numerous
perspectives in nanomagnetism and spintronics
Field-free deterministic ultra fast creation of skyrmions by spin orbit torques
Magnetic skyrmions are currently the most promising option to realize
current-driven magnetic shift registers. A variety of concepts to create
skyrmions were proposed and demonstrated. However, none of the reported
experiments show controlled creation of single skyrmions using integrated
designs. Here, we demonstrate that skyrmions can be generated deterministically
on subnanosecond timescales in magnetic racetracks at artificial or natural
defects using spin orbit torque (SOT) pulses. The mechanism is largely similar
to SOT-induced switching of uniformly magnetized elements, but due to the
effect of the Dzyaloshinskii-Moriya interaction (DMI), external fields are not
required. Our observations provide a simple and reliable means for skyrmion
writing that can be readily integrated into racetrack devices
Emergent Phenomena Induced by Spin-Orbit Coupling at Surfaces and Interfaces
Spin-orbit coupling (SOC) describes the relativistic interaction between the
spin and momentum degrees of freedom of electrons, and is central to the rich
phenomena observed in condensed matter systems. In recent years, new phases of
matter have emerged from the interplay between SOC and low dimensionality, such
as chiral spin textures and spin-polarized surface and interface states. These
low-dimensional SOC-based realizations are typically robust and can be
exploited at room temperature. Here we discuss SOC as a means of producing such
fundamentally new physical phenomena in thin films and heterostructures. We put
into context the technological promise of these material classes for developing
spin-based device applications at room temperature
Inertia-driven resonant excitation of a magnetic skyrmion
Topological spin structures such as magnetic domain walls, vortices, and skyrmions, have been receiving great interest because of their high potential application in various spintronic devices. To utilize them in the future spintronic devices, it is first necessary to understand the dynamics of the topological spin structures. Since inertial effect plays a crucial role in the dynamics of a particle, understanding the inertial effect of topological spin structures is an important task. Here, we report that a strong inertial effect appears steadily when a skyrmion is driven by an oscillating spin-Hall-spintorque (SHST). We find that the skyrmion exhibits an inertia-driven hypocycloid-type trajectory when it is excited by the oscillating SHST. This motion has not been achieved by an oscillating magnetic field, which only excites the breathing mode without the inertial effect. The distinct inertial effect can be explained in terms of a spin wave excitation in the skyrmion boundary which is induced by the non-uniform SHST. Furthermore, the inertia-driven resonant excitation provides a way of experimentally estimating the inertial mass of the skyrmion. Our results therefore pave the way for the development of skyrmion-based device applications
Room temperature chiral magnetic skyrmion in ultrathin magnetic nanostructures
Magnetic skyrmions are chiral spin structures with a whirling configuration.
Their topological properties, nanometer size and the fact that they can be
moved by small current densities have opened a new paradigm for the
manipulation of magnetisation at the nanoscale. To date, chiral skyrmion
structures have been experimentally demonstrated only in bulk materials and in
epitaxial ultrathin films and under external magnetic field or at low
temperature. Here, we report on the observation of stable skyrmions in
sputtered ultrathin Pt/Co/MgO nanostructures, at room temperature and zero
applied magnetic field. We use high lateral resolution X-ray magnetic circular
dichroism microscopy to image their chiral N\'eel internal structure which we
explain as due to the large strength of the Dzyaloshinskii-Moriya interaction
as revealed by spin wave spectroscopy measurements. Our results are
substantiated by micromagnetic simulations and numerical models, which allow
the identification of the physical mechanisms governing the size and stability
of the skyrmions.Comment: Submitted version. Extended version to appear in Nature
Nanotechnolog
Quantum cascade laser frequency stabilisation at the sub-Hz level
Quantum Cascade Lasers (QCL) are increasingly being used to probe the
mid-infrared "molecular fingerprint" region. This prompted efforts towards
improving their spectral performance, in order to reach ever-higher resolution
and precision. Here, we report the stabilisation of a QCL onto an optical
frequency comb. We demonstrate a relative stability and accuracy of 2x10-15 and
10-14, respectively. The comb is stabilised to a remote near-infrared
ultra-stable laser referenced to frequency primary standards, whose signal is
transferred via an optical fibre link. The stability and frequency traceability
of our QCL exceed those demonstrated so far by two orders of magnitude. As a
demonstration of its capability, we then use it to perform high-resolution
molecular spectroscopy. We measure absorption frequencies with an 8x10-13
relative uncertainty. This confirms the potential of this setup for ultra-high
precision measurements with molecules, such as our ongoing effort towards
testing the parity symmetry by probing chiral species
Differential stromal reprogramming in benign and malignant naturally occurring canine mammary tumours identifies disease-modulating stromal components
While cancer-associated stroma (CAS) in malignant tumours is well described, stromal changes in benign forms of naturally occurring tumours remain poorly characterized. Spontaneous canine mammary carcinomas (mCA) are viewed as excellent models of human mCA. We have recently reported highly conserved stromal reprogramming between canine and human mCA based on transcriptome analysis of laser-capture-microdissected FFPE specimen. To identify stromal changes between benign and malignant mammary tumours, we have analysed matched normal and adenoma-associated stroma (AAS) from 13 canine mammary adenomas and compared them to previous data from 15 canine mCA. Our analyses reveal distinct stromal reprogramming even in small benign tumours. While similarities between AAS and CAS exist, the stromal signature clearly distinguished adenomas from mCA. The distinction between AAS and CAS is further substantiated by differential enrichment in several hallmark signalling pathways as well as differential abundance in cellular composition. Finally, we identify COL11A1, VIT, CD74, HLA-DRA, STRA6, IGFBP4, PIGR, and TNIP1 as strongly discriminatory stromal genes between adenoma and mCA, and demonstrate their prognostic value for human breast cancer. Given the relevance of canine CAS as a model for the human disease, our approach identifies disease-modulating stromal components with implications for both human and canine breast cancer
Chemotherapy-induced oral mucositis is associated with detrimental bacterial dysbiosis.
BACKGROUND: Gastrointestinal mucosal injury (mucositis), commonly affecting the oral cavity, is a clinically significant yet incompletely understood complication of cancer chemotherapy. Although antineoplastic cytotoxicity constitutes the primary injury trigger, the interaction of oral microbial commensals with mucosal tissues could modify the response. It is not clear, however, whether chemotherapy and its associated treatments affect oral microbial communities disrupting the homeostatic balance between resident microorganisms and the adjacent mucosa and if such alterations are associated with mucositis. To gain knowledge on the pathophysiology of oral mucositis, 49 subjects receiving 5-fluorouracil (5-FU) or doxorubicin-based chemotherapy were evaluated longitudinally during one cycle, assessing clinical outcomes, bacterial and fungal oral microbiome changes, and epithelial transcriptome responses. As a control for microbiome stability, 30 non-cancer subjects were longitudinally assessed. Through complementary in vitro assays, we also evaluated the antibacterial potential of 5-FU on oral microorganisms and the interaction of commensals with oral epithelial tissues.
RESULTS: Oral mucositis severity was associated with 5-FU, increased salivary flow, and higher oral granulocyte counts. The oral bacteriome was disrupted during chemotherapy and while antibiotic and acid inhibitor intake contributed to these changes, bacteriome disruptions were also correlated with antineoplastics and independently and strongly associated with oral mucositis severity. Mucositis-associated bacteriome shifts included depletion of common health-associated commensals from the genera Streptococcus, Actinomyces, Gemella, Granulicatella, and Veillonella and enrichment of Gram-negative bacteria such as Fusobacterium nucleatum and Prevotella oris. Shifts could not be explained by a direct antibacterial effect of 5-FU, but rather resembled the inflammation-associated dysbiotic shifts seen in other oral conditions. Epithelial transcriptional responses during chemotherapy included upregulation of genes involved in innate immunity and apoptosis. Using a multilayer epithelial construct, we show mucositis-associated dysbiotic shifts may contribute to aggravate mucosal damage since the mucositis-depleted Streptococcus salivarius was tolerated as a commensal, while the mucositis-enriched F. nucleatum displayed pro-inflammatory and pro-apoptotic capacity.
CONCLUSIONS: Altogether, our work reveals that chemotherapy-induced oral mucositis is associated with bacterial dysbiosis and demonstrates the potential for dysbiotic shifts to aggravate antineoplastic-induced epithelial injury. These findings suggest that control of oral bacterial dysbiosis could represent a novel preventive approach to ameliorate oral mucositis
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