53 research outputs found
X-ray absorption spectroscopy and X-ray magnetic circular dichroism studies of transition-metal-co-doped ZnO nano-particles
We report on x-ray absorption spectroscopy (XAS) and x-ray magnetic circular
dichroism (XMCD) studies of the paramagnetic (Mn,Co)-co-doped ZnO and
ferromagnetic (Fe,Co)-co-doped ZnO nano-particles. Both the surface-sensitive
total-electron-yield mode and the bulk-sensitive total-fluorescence-yield mode
have been employed to extract the valence and spin states of the surface and
inner core regions of the nano-particles. XAS spectra reveal that significant
part of the doped Mn and Co atoms are found in the trivalent and tetravalent
state in particular in the surface region while majority of Fe atoms are found
in the trivalent state both in the inner core region and surface region. The
XMCD spectra show that the Fe ions in the surface region give rise to
the ferromagnetism while both the Co and Mn ions in the surface region show
only paramagnetic behaviors. The transition-metal atoms in the inner core
region do not show magnetic signals, meaning that they are
antiferromagnetically coupled. The present result combined with the previous
results on transition-metal-doped ZnO nano-particles and nano-wires suggest
that doped holes, probably due to Zn vacancy formation at the surfaces of the
nano-particles and nano-wires, rather than doped electrons are involved in the
occurrence of ferromagnetism in these systems.Comment: Proceedings of "XAFS theory and nanoparticles
Anisotropic spin-density distribution and magnetic anisotropy of strained LaSrMnO thin films: Angle-dependent x-ray magnetic circular dichroism
Magnetic anisotropies of ferromagnetic thin films are induced by epitaxial
strain from the substrate via strain-induced anisotropy in the orbital magnetic
moment and that in the spatial distribution of spin-polarized electrons.
However, the preferential orbital occupation in ferromagnetic metallic
LaSrMnO (LSMO) thin films studied by x-ray linear dichroism
(XLD) has always been found out-of-plane for both tensile and compressive
epitaxial strain and hence irrespective of the magnetic anisotropy. In order to
resolve this mystery, we directly probed the preferential orbital occupation of
spin-polarized electrons in LSMO thin films under strain by angle-dependent
x-ray magnetic circular dichroism (XMCD). Anisotropy of the spin-density
distribution was found to be in-plane for the tensile strain and out-of-plane
for the compressive strain, consistent with the observed magnetic anisotropy.
The ubiquitous out-of-plane preferential orbital occupation seen by XLD is
attributed to the occupation of both spin-up and spin-down out-of-plane
orbitals in the surface magnetic dead layer.Comment: 20 pages, 4 figure
The predictive value of p53, p53R2, and p21 for the effect of chemoradiation therapy on oesophageal squamous cell carcinoma
The p53 family regulates cell-cycle arrest, triggers apoptosis or is involved in repair of DNA damage. In the present study, we analysed the expression of some p53 family proteins and their responses to chemoradiation therapy (CRT) in cases of oesophageal squamous cell carcinoma (ESCC). We immunohistochemically investigated the relationship between p53, p53R2, and p21 expression in biopsy specimens of untreated primary tumours and their clinical and histological responses to CRT in 62 patients with ESCC. Chemoradiation therapy consisted of 5-fluorouracil plus cisplatin and 40 Gy of radiation. The rates of clinical and histological responses (complete or partial) to CRT were 71.0% (clinical) and 52.8% (histological). The rate of positive expression was 43.5% for p53, 37.1% for p53R2, and 54.8% for p21 expression. Statistically significant correlations were found between p53 or p53R2 expression and favourable response to CRT (P=0.0001 or 0.041 clinical, P=0.016 or 0.0018 histological, respectively). Furthermore, in p53-negative tumours, CRT was more effective in tumours with p53R2 negative expression than those with p53R2 positive expression (P=0.0014). We demonstrated that the negative expression of p53 and p53R2 expression was closely related to the effect of CRT and should predict the CRT outcome in patients with ESCC
Development of Mouse Hepatocyte Lines Permissive for Hepatitis C Virus (HCV)
The lack of a suitable small animal model for the analysis of hepatitis C virus (HCV) infection has hampered elucidation of the HCV life cycle and the development of both protective and therapeutic strategies against HCV infection. Human and mouse harbor a comparable system for antiviral type I interferon (IFN) induction and amplification, which regulates viral infection and replication. Using hepatocytes from knockout (ko) mice, we determined the critical step of the IFN-inducing/amplification pathways regulating HCV replication in mouse. The results infer that interferon-beta promoter stimulator (IPS-1) or interferon A receptor (IFNAR) were a crucial barrier to HCV replication in mouse hepatocytes. Although both IFNARko and IPS-1ko hepatocytes showed a reduced induction of type I interferons in response to viral infection, only IPS-1-/- cells circumvented cell death from HCV cytopathic effect and significantly improved J6JFH1 replication, suggesting IPS-1 to be a key player regulating HCV replication in mouse hepatocytes. We then established mouse hepatocyte lines lacking IPS-1 or IFNAR through immortalization with SV40T antigen. Expression of human (h)CD81 on these hepatocyte lines rendered both lines HCVcc-permissive. We also found that the chimeric J6JFH1 construct, having the structure region from J6 isolate enhanced HCV replication in mouse hepatocytes rather than the full length original JFH1 construct, a new finding that suggests the possible role of the HCV structural region in HCV replication. This is the first report on the entry and replication of HCV infectious particles in mouse hepatocytes. These mouse hepatocyte lines will facilitate establishing a mouse HCV infection model with multifarious applications
Biomedical and therapeutic applications of biosurfactants
During the last years, several applications of biosurfactants with medical purposes have been reported. Biosurfactants are considered relevant molecules for applications in combating many diseases and as therapeutic agents due to their antibacterial, antifungal and antiviral activities. Furthermore, their role as anti-adhesive agents against several pathogens illustrate their utility as suitable anti-adhesive coating agents for medical insertional materials leading to a reduction of a large number of hospital infections without the use of synthetic drugs and chemicals. Biomedical and therapeutic perspectives of biosurfactants applications are presented and discussed in this chapter
Comparative Pathogenesis of an Avian H5N2 and a Swine H1N1 Influenza Virus in Pigs
Pigs are considered intermediate hosts for the transmission of avian influenza viruses (AIVs) to humans but the basic organ pathogenesis of AIVs in pigs has been barely studied. We have used 42 four-week-old influenza naive pigs and two different inoculation routes (intranasal and intratracheal) to compare the pathogenesis of a low pathogenic (LP) H5N2 AIV with that of an H1N1 swine influenza virus. The respiratory tract and selected extra-respiratory tissues were examined for virus replication by titration, immunofluorescence and RT-PCR throughout the course of infection. Both viruses caused a productive infection of the entire respiratory tract and epithelial cells in the lungs were the major target. Compared to the swine virus, the AIV produced lower virus titers and fewer antigen positive cells at all levels of the respiratory tract. The respiratory part of the nasal mucosa in particular showed only rare AIV positive cells and this was associated with reduced nasal shedding of the avian compared to the swine virus. The titers and distribution of the AIV varied extremely between individual pigs and were strongly affected by the route of inoculation. Gross lung lesions and clinical signs were milder with the avian than with the swine virus, corresponding with lower viral loads in the lungs. The brainstem was the single extra-respiratory tissue found positive for virus and viral RNA with both viruses. Our data do not reject the theory of the pig as an intermediate host for AIVs, but they suggest that AIVs need to undergo genetic changes to establish full replication potential in pigs. From a biomedical perspective, experimental LP H5 AIV infection of pigs may be useful to examine heterologous protection provided by H5 vaccines or other immunization strategies, as well as for further studies on the molecular pathogenesis and neurotropism of AIVs in mammals
- …