1,273 research outputs found

    Electrochemical synthesis and properties of CoO2, the x = 0 phase of the AxCoO2 systems (A = Li, Na)

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    Single-phase bulk samples of the "exotic" CoO2, the x = 0 phase of the AxCoO2 systems (A = Li, Na), were successfully synthesized through electrochemical de-intercalation of Li from pristine LiCoO2 samples. The samples of pure CoO2 were found to be essentially oxygen stoichiometric and possess a hexagonal structure consisting of stacked triangular-lattice CoO2 layers only. The magnetism of CoO2 is featured with a temperature-independent susceptibility of the magnitude of 10-3 emu/mol Oe, being essentially identical to that of a Li-doped phase, Li0.12CoO2. It is most likely that the CoO2 phase is a Pauli-paramagnetic metal with itinerant electrons.Comment: 12 pages, 3 figure

    Field induced long-range-ordering in an S=1 quasi-one-dimensional Heisenberg antiferromagnet

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    We have measured the heat capacity and magnetization of the spin one one-dimensional Heisenberg antiferromagnet NDMAP and constructed a magnetic field versus temperature phase diagram. We found a field induced long-range magnetic ordering. We have been successful in explaining the phase diagram theoretically.Comment: 6 pages, 18 figure

    Electrochemical synthesis and properties of CoO[sub 2], the x=0 phase of the A[sub x]CoO[sub 2] systems (A=Li,Na)

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    Single-phase bulk samples of the “exotic” CoO2, the x=0 phase of the AxCoO2 systems (A=Li,Na), were successfully synthesized through electrochemical deintercalation of Li from pristine LiCoO2 samples. The samples of pure CoO2 were found to be essentially oxygen stoichiometric and possess a hexagonal structure consisting of stacked triangular-lattice CoO2 layers only. The magnetism of CoO2 is featured with a temperature-independent susceptibility of the magnitude of 10−3emu/molOe, being essentially identical to that of a Li-doped phase, Li0.12CoO2. It is most likely that the CoO2 phase is a Pauli-paramagnetic metal with itinerant electrons.Peer reviewe

    High-field phase diagram of the Haldane-gap antiferromagnet Ni(C5H14N2)2N3(PF6)Ni (C_5 H_{14} N_2)_2 N_3 (PF_6)

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    We have determined the magnetic phase diagram of the quasi-one-dimensional S=S= 1 Heisenberg antiferromagnet Ni(C5H14N2)2N3(PF6)Ni (C_5 H_{14} N_2)_2 N_3 (PF_6) by specific heat measurements to 150 mK in temperature and 32 T in magnetic field. When field is applied along the spin-chain direction, a new phase appears at Hc214H_{c2}\approx 14 T. For the previously known phases of field-induced order, accurate determination is made of the power-law exponents of the ordering temperature near the zero-temperature critical field HcH_c, owing to the four-fold improvement of the minimum temperature over the previous work. The results are compared with the predictions based on the Bose-Einstein condensation of triplet excitations. Substituting deuterium for hydrogen is found to slightly reduce the interchain exchange.Comment: 6 pages, 6 figure

    Field-induced long-range order in the S=1 antiferromagnetic chain

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    The quasi-one dimensional S=1 antiferromagnet in magnetic field H is investigated with the exact diagonalization of finite chains and the mean field approximation for the interchain interaction. In the presence of the single-ion anisotropy D, the full phase diagram in the HTHT plane is presented for H \parallel D and H \perp D. The shape of the field-induced long-range ordered phase is revealed to be quite different between the two cases, as observed in the recent experiment of NDMAP. The estimated ratio of the interchain and intrachain couplings of NDMAP (J'/J ~ 10^{-3}) is consistent with the neutron scattering measurement.Comment: 4 pages, Revtex, with 6 eps figure

    Haldane-gap excitations in the low-H_c 1-dimensional quantum antiferromagnet NDMAP

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    Inelastic neutron scattering on deuterated single-crystal samples is used to study Haldane-gap excitations in the new S=1 one-dimensional quantum antiferromagnet NDMAP, that was recently recognized as an ideal model system for high-field studies. The Haldane gap energies Δx=0.42\Delta_x=0.42 meV, Δy=0.52\Delta_y=0.52 meV and Δz=1.86\Delta_z=1.86 meV, for excitations polarized along the a, b, and c crystallographic axes, respectively, are directly measured. The dispersion perpendicular to the chain axis c is studied, and extremely weak inter-chain coupling constants Jy=1.8103J_y=1.8\cdot 10^{-3} meV and Jx=3.5104J_x=3.5\cdot 10^{-4} meV, along the a and b axes, respectively, are determined. The results are discussed in the context of future experiments in high magnetic fields.Comment: 5 pages, 4 figures, submitted to Phys. Rev.

    Dichotomous Scoring of TDP-43 Proteinopathy from Specific Brain Regions in 27 Academic Research Centers: Associations with Alzheimer\u27s Disease and Cerebrovascular Disease Pathologies

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    TAR-DNA binding protein 43 (TDP-43) proteinopathy is a common brain pathology in elderly persons, but much remains to be learned about this high-morbidity condition. Published stage-based systems for operationalizing disease severity rely on the involvement (presence/absence) of pathology in specific anatomic regions. To examine the comorbidities associated with TDP-43 pathology in aged individuals, we studied data from the National Alzheimer’s Coordinating Center (NACC) Neuropathology Data Set. Data were analyzed from 929 included subjects with available TDP-43 pathology information, sourced from 27 different American Alzheimer’s Disease Centers (ADCs). Cases with relatively unusual diseases including autopsy-proven frontotemporal lobar degeneration (FTLD-TDP or FTLD-tau) were excluded from the study. Our data provide new information about pathologic features that are and are not associated with TDP-43 pathologies in different brain areas—spinal cord, amygdala, hippocampus, entorhinal cortex/inferior temporal cortex, and frontal neocortex. Different research centers used cite-specific methods including different TDP-43 antibodies. TDP-43 pathology in at least one brain region was common (31.4%) but the pathology was rarely observed in spinal cord (1.8%) and also unusual in frontal cortex (5.3%). As expected, TDP-43 pathology was positively associated with comorbid hippocampal sclerosis pathology and with severe AD pathology. TDP-43 pathology was also associated with comorbid moderate-to-severe brain arteriolosclerosis. The association between TDP-43 pathology and brain arteriolosclerosis appears relatively specific since there was no detected association between TDP-43 pathology and microinfarcts, lacunar infarcts, large infarcts, cerebral amyloid angiopathy (CAA), or circle of Willis atherosclerosis. Together, these observations provide support for the hypothesis that many aged brains are affected by a TDP-43 proteinopathy that is more likely to be seen in brains with AD pathology, arteriolosclerosis pathology, or both
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