RESUMO
Kagomé lattice magnets have emerged as a versatile platform on which to discover and explore the underlying physics of quantum-spin liquids and related states of matter, although experimental examples of ideal kagomé lattices remain rare. Here we report that Na2Ti3Cl8 is an ideal realization of an insulating S = 1 kagomé magnet. This material undergoes a discrete two-step trimerization upon cooling, transforming from a centrosymmetric, paramagnetic high-temperature (HT) R3m phase to noncentrosymmetric, polar, and trimerized intermediate- (IT) and low-temperature (LT) R3m phases via two successive first-order phase transitions. Symmetry mode decomposition analysis shows that trimerization requires activation of the proper polar order parameter Γ2- and that this mode becomes active at the HT â IT phase transition. The magnitude of this order parameter approximately doubles at the IT â LT transition, with possible activation of a second polar mode, corresponding to Na2 and Ti3Cl8 displacing layers toward each other, at the IT â LT transition. Specific heat measurements reveal comparable changes in entropy between the LT â IT transition, 18.6(1.0) J (mol of f.u.)-1 K-1, and the IT â LT transition, 16.8(1.0) J (mol of f.u.)-1 K-1, demonstrating loss of the magnetic degrees of freedom and constraining possible models for the magnetic and electronic structures of the IT and LT phases. Thus, Na2Ti3Cl8 demonstrates a novel mechanism to obtain polar structures driven by geometrically frustrated lattices and metal-metal bonding and highlights the rich physics arising from kagomé lattice materials.
RESUMO
The synthesis and physical properties of the K(1-x)Ir4O8 (0 ≤ x ≤ 0.7) solid solution are reported. The structure of KIr4O8, solved with single-crystal X-ray diffraction at T = 110 K, is found to be tetragonal, space group I4/m, with a = 10.0492(3) Å and c = 3.14959(13) Å. A highly anisotropic displacement parameter is found for the potassium cation. Density functional theory calculations suggest that this anisotropy is due to a competition between atomic size and bond valence. KIr4O8 has a significant electronic contribution to the specific heat, γ = 13.9 mJ mol-Ir(-1) K(-2), indicating an effective carrier mass of m*/me ≈ 10. Further, there is a magnetic-field-dependent upturn in the specific heat at T < 3 K, suggestive of a magnetically sensitive phase transition below T < 1.8 K. Resistivity and magnetization measurements show that both end-members of the solid solution, KIr4O8 and K(1-x)Ir4O8 (x ≈ 0.7), are metallic, with no significant trends in the temperature-independent contributions to the magnetization. These results are interpreted and discussed in the context of the importance of the variability of the oxidation state of iridium. The differences in physical properties between members of the K(1-x)Ir4O8 (0 ≤ x ≤ 0.7) series are small and appear to be insensitive to the iridium oxidation state.
RESUMO
BACKGROUND: Langerhans cells (LCs) are antigen-presenting dendritic cells located in the skin. It has been reported that LC activation is associated with painful diabetic neuropathy (PDN); however, the mechanism of LC activation is still unclear. METHODS: The db/db mouse, a rodent model of PDN, was used to study the roles of LCs in the development of PDN in type 2 diabetes. Hind foot pads from db/db and control db/+ mice from 5 to 24 weeks of age (encompassing the period of mechanical allodynia development and its abatement) were collected and processed for immunohistochemistry studies. LCs were identified with immunohistochemistry using an antibody against CD207 (Langerin). The intraepidermal nerve fibers and subepidermal nerve plexus were identified by immunohistochemistry of protein gene product 9.5 (PGP 9.5) and tropomyosin-receptor kinase (Trk) A, the high affinity nerve growth factor receptor. RESULTS: CD207-positive LCs increased in the db/db mouse during the period of mechanical allodynia, from 8 to 10 weeks of age, in both the epidermis and subepidermal plexus. At 16 weeks of age, when mechanical allodynia diminishes, LC populations were reduced in the epidermis and subepidermal plexus. Epidermal LCs (ELCs) were positive for Trk A. Subepidermal LCs (SLCs) were positive for CD68, suggesting that they are immature LCs. Additionally, these SLCs were positive for the receptor of advanced glycation end products (RAGE) and were in direct contact with TNF-α-positive nerve fibers in the subepidermal nerve plexus during the period of mechanical allodynia. Intrathecal administration of SB203580, a p38 kinase inhibitor, significantly reduced mechanical allodynia, TNF-α expression in the subepidermal plexus, and increased both ELC and SLC populations during the period of mechanical allodynia. CONCLUSIONS: Our data support the hypothesis that increased LC populations in PDN are activated by p38-dependent neurogenic factors and may be involved in the pathogenesis of PDN.