Insight into the biological effects of acupuncture points by X-ray absorption fine structure.

Exploration of the biological effects of transition metal ions in acupuncture points is essential to clarify the functional mechanism of acupuncture treatment. Here we show that in the SP6 acupuncture point (Sanyinjiao) the Fe ions are in a high-spin state of approximately t2g4.5eg1.5 in an Fe-N(O) octahedral crystal field. The Fe K-edge synchrotron radiation X-ray absorption fine structure results reveal that the Fe-N and Fe-O bond lengths in the SP6 acupuncture point are 2.05 and 2.13 Å, respectively, and are 0.05-0.10 Å longer than those in the surrounding tissue. The distorted atomic structure reduces the octahedral symmetry and weakens the crystal field around the Fe ions by approximately 0.3 eV, leading to the high-spin configuration of the Fe ions, which is favorable for strengthening the magnetotransport and oxygen transportation properties in the acupuncture point by the enhanced spin coherence. This finding might provide some insight into the microscopic effect of the atomic and electronic interactions of transition metal ions in the acupuncture point. Graphical Abstract ᅟ.

Fast Photoelectron Transfer in (Cring)-C3N4 Plane Heterostructural Nanosheets for Overall Water Splitting.

Direct and efficient photocatalytic water splitting is critical for sustainable conversion and storage of renewable solar energy. Here, we propose a conceptual design of two-dimensional C3N4-based in-plane heterostructure to achieve fast spatial transfer of photoexcited electrons for realizing highly efficient and spontaneous overall water splitting. This unique plane heterostructural carbon ring (Cring)-C3N4 nanosheet can synchronously expedite electron-hole pair separation and promote photoelectron transport through the local in-plane π-conjugated electric field, synergistically elongating the photocarrier diffusion length and lifetime by 10 times relative to those achieved with pristine g-C3N4. As a result, the in-plane (Cring)-C3N4 heterostructure could efficiently split pure water under light irradiation with prominent H2 production rate up to 371 µmol g-1 h-1 and a notable quantum yield of 5% at 420 nm.

Oxyhydroxide Nanosheets with Highly Efficient Electron-Hole Pair Separation for Hydrogen Evolution.

The facile electron-hole pair recombination in earth-abundant transition-metal oxides is a major limitation for the development of highly efficient hydrogen evolution photocatalysts. In this work, the thickness of a layered ß-CoOOH semiconductor that contains metal/hydroxy groups was reduced to obtain an atomically thin, two-dimensional nanostructure. Analysis by ultrafast transient absorption spectroscopy revealed that electron-hole recombination is almost suppressed in the as-prepared 1.3 nm thick ß-CoOOH nanosheet, which leads to prominent electron-hole separation efficiencies of 60-90 % upon irradiation at 350-450 nm, which are ten times higher than those of the bulk counterpart. X-ray absorption spectroscopy and first-principles calculations demonstrate that [HO-CoO6-x] species on the nanosheet surface promote H(+) adsorption and H2 desorption. An aqueous suspension of the ß-CoOOH nanosheets exhibited a high hydrogen production rate of 160 µmol g(-1) h(-1) even when the system was operated for hundreds of hours.

CoOOH Nanosheets with High Mass Activity for Water Oxidation.

Endowing transition-metal oxide electrocatalysts with high water oxidation activity is greatly desired for production of clean and sustainable chemical fuels. Here, we present an atomically thin cobalt oxyhydroxide (γ-CoOOH) nanosheet as an efficient electrocatalyst for water oxidation. The 1.4 nm thick γ-CoOOH nanosheet electrocatalyst can effectively oxidize water with extraordinarily large mass activities of 66.6 A g(-1), 20 times higher than that of γ-CoOOH bulk and 2.4 times higher than that of the benchmarking IrO2 electrocatalyst. Experimental characterizations and first-principles calculations provide solid evidence to the half-metallic nature of the as-prepared nanosheets with local structure distortion of the surface CoO(6-x) octahedron. This greatly enhances the electrophilicity of H2O and facilitates the interfacial electron transfer between Co ions and adsorbed -OOH species to form O2, resulting in the high electrocatalytic activity of layered CoOOH for water oxidation.

Realizing ferromagnetic coupling in diluted magnetic semiconductor quantum dots.

Manipulating the ferromagnetic interactions in diluted magnetic semiconductor quantum dots (DMSQDs) is a central theme to the development of next-generation spin-based information technologies, but this remains a great challenge because of the intrinsic antiferromagnetic coupling between impurity ions therein. Here, we propose an effective approach capable of activating ferromagnetic exchange in ZnO-based DMSQDs, by virtue of a core/shell structure that engineers the energy level of the magnetic impurity 3d levels relative to the band edge. This idea has been successfully applied to Zn(0.96)Co(0.04)O DMSQDs covered by a shell of ZnS or Ag2S. First-principles calculations further indicate that covering a ZnS shell around the Co-doped ZnO core drives a transition of antiferromagnetic-to-ferromagnetic interaction, which occurs within an effective depth of 1.2 nm underneath the surface in the core. This design opens up new possibility for effective manipulation of exchange interactions in doped oxide nanostructures for future spintronics applications.

Scattering imaging method in transmission x-ray microscopy.

We present a x-ray microscopy technique based on structured illumination in a microscope that characterizes the size of the subresolution-limit features. The technique is effective for characterizing fine structures substantially beyond the Rayleigh resolution of the microscope. We carried out optical experiments to demonstrate the basic principle of this new technique. Experimental results show good agreement with theoretical predictions. This technique should find a wide range of important imaging applications with a feature size down to nanometer scale, such as oil and gas reservoir rocks, advanced composites, and functional nanodevices and materials.

Microstructure and gas-sensing property of the ordered mesoporous Co3O4.

We report the microstructure, gas-sensing properties of the ordered mesoporous Co3O4 prepared by modified KIT-6 template method. Highly ordered mesoporous nanostructures of the as-prepared products have been characterized by X-ray diffraction (XRD), extended X-ray absorption fine structure (EXAFS), high-resolution transmission electron microscopy (HRTEM) and N2 adsorption/desorption analysis. We find that the ordered mesoporous Co3O4 enables a significant improvement of sensor response and selectivity to ethanol, which demonstrates the potential use of the ordered mesoporous Co3O4 as alcohol gas-sensing material. Through the analysis of microstructure including HRTEM and N2 adsorption/desorption, the sensing properties for the ordered mesoporous Co3O4 can be attributed qualitatively to its large specific surface area and porous morphology. Moreover, the results of EXAFS illustrate that the disorder degree and unsaturated bond of the ordered mesoporous Co3O4 increase, which agree well with the results observed in gas sensors. This makes the nanostructured ordered mesoporous Co3O4 a promising sensor material for detecting the alcohol gas.

Probing nucleation pathways for morphological manipulation of platinum nanocrystals.

Understanding the formation process in the controlled synthesis of nanocrystals will lead to the effective manipulation of the morphologies and properties of nanomaterials. Here, in-situ UV-vis and X-ray absorption spectroscopies are combined to monitor the tracks of the nucleation pathways in the solution synthesis of platinum nanocrystals. We find experimentally that the control over nucleation pathways through changing the strength of reductants can be efficiently used to manipulate the resultant nanocrystal shapes. The in-situ measurements show that two different nucleation events involving the formation of one-dimensional "Pt(n)Cl(x)" complexes from the polymerization of linear "Cl(3)Pt-PtCl(3)" dimers and spherical "Pt(n)(0)" clusters from the aggregation of Pt(0) atoms occur for the cases of weak and strong reductants; and the resultant morphologies are nanowires and nanospheres, respectively. This study provides a crucial insight into the correlation between the particle shapes and nucleation pathways of nanomaterials.

High-speed X-ray microscopy by use of high-resolution zone plates and synchrotron radiation.

X-ray microscopy based on synchrotron radiation has become a fundamental tool in biology and life sciences to visualize the morphology of a specimen. These studies have particular requirements in terms of radiation damage and the image exposure time, which directly determines the total acquisition speed. To monitor and improve these key parameters, we present a novel X-ray microscopy method using a high-resolution zone plate as the objective and the matching condenser. Numerical simulations based on the scalar wave field theory validate the feasibility of the method and also indicate the performance of X-ray microscopy is optimized most with sub-10-nm-resolution zone plates. The proposed method is compatible with conventional X-ray microscopy techniques, such as computed tomography, and will find wide applications in time-resolved and/or dose-sensitive studies such as living cell imaging.

Use of fractal zone plates for transmission X-ray microscopy.

In this contribution we discuss the possibility of designing a modified transmission X-ray microscope by using fractal zone plates (Fzps) as diffractive optical elements. In the modified transmission X-ray microscope optical layout, we first introduced a fractal zone plate as the microscope objective. Indeed, a fractal zone plate cannot only be used as an image-forming component but also as a condenser element to achieve an extended depth of field. Numerical analysis reveals that fractal zone plates and conventional Fresnel zone plates have similar imaging capabilities under different coherent illumination. Using a fractal zone plate as a condenser we also simulated axial irradiance. Results confirm that fractal zone plates can improve focusing capability with an extended depth of field. Although preliminary, these simulations clearly reveal that fractal zone plates, when available, will be of great help in microscope layouts, in particular for foreseen high-resolution applications in the "water window" as strongly required in biological research.

Metal-insulator transition in V(1-x)W(x)O2: structural and electronic origin.

The driving mechanism of the metal-insulator transition (MIT) in VO(2) has always attracted attention, in particular with regards to understanding if and how the doping mechanism may tune the MIT transition temperature. However, due to the lack of detailed local structural information, in this oxide the underlying MIT mechanism is still matter of debate. In this contribution on the V(1-x)W(x)O(2) system, we attempt to clarify the origin of the MIT induced by tungsten doping. Combining W L(3)-edge and V K-edge extended X-ray absorption fine-structure (EXAFS) spectroscopy, the local structures around both V and W have been obtained. The data point out the occurrence of internal stress along the V-V chains induced by doping. It reaches a critical value that remains constant during the transition. The main effect of the internal stress on the vanadium local structure has also been identified. Actually, upon increasing the dopant concentration, the tilt of the V-V pairs towards the apex oxygen atoms in the VO(6) octahedron decreases while the V-V bond lengths remain unchanged. The electronic structure has also been investigated by O K-edge X-ray absorption near-edge structure (XANES) spectroscopy. Actually, at high doping concentrations the interaction of O(2p) and the V d(∥) state increases, while the hybridization of O(2p) and V π* decreases. The O(2p)-V(3d) hybridization is therefore an essential parameter correlated with the decreasing transition temperature in the V(1-x)W(x)O(2) system.

Insights into initial kinetic nucleation of gold nanocrystals.

Understanding the initial nucleation mechanism of monodisperse nanocrystals (NCs) during synthesis process is an important prerequisite to control the desired sizes and to manipulate the properties of nanoscale materials. The acquisition of information for the small nanocluster nucleation process, however, still remains challenging. Here, using a continuous-flow in situ X-ray absorption fine structure (XAFS) spectroscopy for time-resolved studies, we have clarified the initial kinetic nucleation of Au clusters under the grain size of 1 nm for the classical Au NCs synthesis via the reduction of AuCl(4)(-) in aqueous solution. The in situ XAFS results present the experimental revelation of the formation of intermediate Cl(3)(-)Au-AuCl(3)(-) dimer and the subsequent higher complexes 'Au(n)Cl(n+x)' in the initial nucleation stage. We propose a kinetic three-step mechanism involving the initial nucleation, slow growth, and eventual coalescence for the Au NCs formation, which may be helpful for the synthesis of metallic nanomaterials.

Binding and inhibition of copper ions to RecA inteins from Mycobacterium tuberculosis.

Protein splicing is a unique post-translational process in which an intein excises itself from a precursor with the concomitant ligation of flanking sequences. The binding of zinc to intein inhibits protein splicing reversibly and EDTA relieves the inhibition. Copper was found to inhibit protein trans splicing; however, the recovery of intein splicing required both EDTA and TCEP, suggesting a different inhibition mechanism for copper compared to zinc. In this work, we have investigated the binding properties and inhibition effects of copper ions on the RecA intein from Mycobacterium tuberculosis. Both Cu(+) and Cu(2+) exhibited high binding affinity to inteins, while different binding sites were identified. Cu(2+) coordinates to Cys1, the key residue involved in the mechanism of protein splicing, however, Cu(+) does not coordinate to cysteine. An in vitro inhibition assay indicated that monovalent Cu(+) demonstrates reversible inhibition to protein splicing, and the inhibitory efficiency is comparable to Zn(2+). Redox reaction between Cu(2+) and cysteine in inteins were observed and the rate constants were determined. The results suggested a dual role for Cu(2+) in the inhibition of intein splicing: strong coordination of Cu(2+) to key residues (including Cys1) in the intein, and subsequent oxidation of Cys1, the residue required for the N-->S acyl shift step in protein splicing. A kinetic study suggested that the coordination could be the major cause of inhibition effect of Cu(2+) initially, whereas the redox reaction could play an additional role in inhibition at a later stage.

Up-regulation of FAT4 enhances the chemosensitivity of colorectal cancer cells treated by 5-FU.

BACKGROUND: Colorectal cancer (CRC) has high mortality, and 5-fluorouracil (5-FU) is a common clinical chemotherapeutic drug. The current study aimed to investigate the role of FAT4 in chemosensitivity of CRC cells treated by 5-FU. METHODS: The immunohistochemistry and qRT-PCR was conducted to measure the FAT4 expression in CRC and adjacent tissues. The FAT4 expression was determined by qRT-PCR and Western blot, comparison of FAT expression between normal and several CRC cell lines was then made, so as to identify cell lines with the highest (LS174T) and the lowest (SW-620) expressions of FAT4. The effects of 5-FU stimulation at various doses on cell viability were determined by CCK-8, and the level of FAT4 was also measured. After FAT4 knockdown in LS174T or FAT4 overexpression in SW-620 with or without pretreatment of 5-FU (30 µg/mL), cell growth, colony formation, cell migration and invasion, angiogenesis were determined by flow cytometry, wound-healing, transwell assay and tube formation assay, respectively. The expression levels of epithelial-mesenchymal transition (EMT) markers were detected by qRT-PCR and Western blot. RESULTS: FAT4 was down-regulated in CRC tissues and cells, cell viability of CRC cells was decreased. The level of FAT4 was increased with the increase of 5-FU concentrations. Moreover, 5-FU stimulation increased FAT4 expression, and reduced cell proliferation, migration, invasion, angiogenesis and cell EMT process, furthermore, such effects of 5-FU stimulation could be enhanced by FAT4 overexpression but reversed by FAT4 knockdown. CONCLUSIONS: Upregulation of FAT4 could increase the sensitivity of CRC cells to 5-FU.

Spectroscopic characteristics of differently produced single-walled carbon nanotubes.

Single-walled carbon nanotubes (SWNTs) synthesized with different methods are investigated by using multiple characterization techniques, including Raman scattering, optical absorption, and X-ray absorption near edge structure, along with X-ray photoemission by following the total valence bands and C 1s core-level spectra. Four different SWNT materials (produced by arc discharge, HiPco, laser ablation, and CoMoCat methods) contain nanotubes with diameters ranging from 0.7 to 2.8 nm. The diameter distribution and the composition of metallic and semiconducting tubes of the SWNT materials are strongly affected by the synthesis method. Similar sp(2) hybridization of carbon in the oxygenated SWNT structure can be found, but different surface functionalities are introduced while the tubes are processed. All the SWNTs demonstrate stronger plasmon resonance excitations and lower electron binding energy than graphite and multiwalled carbon nanotubes. These SWNT materials also exhibit different valence-band X-ray photoemission features, which are considerably affected by the nanotube diameter distribution and metallic/semiconducting composition.

Effect of STC2 gene silencing on colorectal cancer cells.

Stanniocalcin 2 (STC2), a secretory glycoprotein hormone, regulates many biological processes including cell proliferation, apoptosis, tumorigenesis and atherosclerosis. However, the effect of STC2 on proliferation, migration and epithelial­mesenchymal transition (EMT) progression in human colorectal cancer (CRC) cells remains poorly understood. The expression level of STC2 was determined by quantitative real­time polymerase chain reaction (qPCR) and western blot analysis. Cell Counting Kit­8 (CCK­8) was used to detect the viability of SW480 cells. The invasion and migration of cells were identified by wound healing and Transwell assays. The mRNA and protein expression levels of ß­catenin, matrix metalloproteinase (MMP)­2, MMP­9, E­cadherin and vimentin were assessed by qPCR and western blot analysis. In the present study, it was demonstrated that STC2 was highly expressed in the CRC cell lines. After silencing of STC2, the cell viability, migration and invasion were significantly reduced. Silencing of STC2 in the CRC Sw480 cells increased the expression of E­cadherin and decreased the expression of vimentin, MMP­2 and MMP­9, compared to those in the normal and empty vector group. Furthermore, the expression of ß­catenin in the STC2 gene silenced group was suppressed, and the expression of ß­catenin was reversed by Wnt activator, SB216763. These results demonstrated that STC2 participates in the development and progression of CRC by promoting CRC cell proliferation, survival and migration and activating the Wnt/ß­catenin signaling pathway.

Rifampicin Resistance and Multidrug-Resistant Tuberculosis Detection Using Xpert MTB/RIF in Wuhan, China: A Retrospective Study.

BACKGROUND: The Xpert MTB/RIF test (Cepheid, Sunnyvale, CA) can simultaneously detect the Mycobacterium tuberculosis (MTB) complex DNA and rifampicin (RFP) resistance and can rapidly determine RFP resistance and predict multidrug-resistant tuberculosis (MDR-TB). In this study, we analyzed clinical examination results of a hospital specializing in TB treatment in Wuhan, Hubei, China, and examined the use of traditional culture and drug-sensitive test (DST) results as a gold standard to assess the diagnosis value of the Xpert MTB/RIF test in RFP resistance and MDR-TB. MATERIALS AND METHODS: A total of 2,910 specimens were received in the Mycobacteriology Laboratory, Wuhan Pulmonary Hospital, for Xpert MTB/RIF testing between December 2013 and December 2014. After the results were reviewed by exclusion criteria, 1,066 Xpert test results were eligible for our study. We then compared the Xpert test results with sputum acid-fast bacilli staining, cultures, and DST results. RESULTS: In total, Xpert correctly identified 96.71% (147/152) RFP-resistant TB and 98.25% (898/914) RFP-sensitive TB specimens. Of the 147 RFP-resistant TB specimens detected by Xpert, 122 MDR-TB (82.99%) were identified by traditional culture and DST techniques. CONCLUSIONS: Xpert can simultaneously detect MTB and RFP resistance with high sensitivity and specificity. Thus, Xpert testing aids in saving a considerable amount of time in the diagnosis and treatment of MDR-TB.

Curcumin protects against liver fibrosis by attenuating infiltration of Gr1hi monocytes through inhibition of monocyte chemoattractant protein-1.

BACKGROUND AND AIMS: Liver fibrosis is concomitant with monocyte infiltration, which has been highlighted as novel therapeutic targets for chronic liver diseases. We aimed to investigate whether curcumin might protect the liver from carbon tetrachloride (CCl4)-induced fibrosis by attenuating the recruitment of Gr1hi monocytes through inhibition of monocyte chemoattractant protein-1 (MCP-1). METHODS: Mice were intraperitoneally injected with CCl4 to induce liver fibrosis. Curcumin was orally administrated to mice. Hepatic inflammation and fibrosis were evaluated by analysis of liver function and hepatic histopathology. Infiltration of the Gr1hi monocytes was assessed by flow cytometry and immunohistochemistry. Moreover, mRNA expression levels of tumor necrosis factor (TNF)-α, interleukin (IL)-6, IL-1ß, and transforming growth factor (TGF)-ß1 were determined by real time PCR. Hepatic expression of MCP-1 was determined by real time PCR and immunohistochemistry. RESULTS: Curcumin significantly attenuated inflammation and fibrosis, as revealed by histological and biochemical analysis. The intrahepatic infiltration of Gr1hi monocytes was attenuated by curcumin administration. T cells, NK cells, NKT cells, and dendritic cells were not affected by curcumin. Curcumin significantly reduced the expression of TNF-α and TGF-ß1, which is in line with the decreased numbers of intrahepatic Gr1hi monocytes. Intrahepatic MCP-1 expression of CCl4-challenged mice was inhibited by curcumin. CONCLUSIONS: The anti-inflammatory and antifibrotic effects of curcumin could be contributed to its prevention of Gr1hi monocyte infiltration into the injured livers through inhibition of MCP-1. These new findings extend our understanding on the mechanisms of the anti-inflammatory and antifibrotic effects of curcumin.

Increase of infiltrating monocytes in the livers of patients with chronic liver diseases.

Infiltrating monocytes have been demonstrated to contribute to tissue damage in experimental models of liver injury and fibrosis. However, less is known about monocyte infiltration in the livers of patients with chronic liver diseases (CLD). In the present study, we demonstrated that CD68+ hepatic macrophages and MAC387+ infiltrating monocytes were significantly increased in the livers of CLD patients with different etiologies as compared with normal liver tissue. In addition, CLD patients with higher inflammatory grading scores had more CD68+ macrophages and MAC387+ monocytes infiltration in their livers compared to those with lower scores. Significantly more MAC387+ infiltrating monocytes were found in the liver tissue of CLD patients with higher fibrotic staging scores compared to those with lower scores. Monocyte chemoattractant protein-1 (MCP-1) expression was significantly increased in the livers of CLD patients with different etiologies. MCP-1 staining scores were significantly positively associated with the numbers of MAC387+ infiltrating monocytes in CLD patients. Taken together, our results demonstrate that infiltrating monocytes may play a pathological role in exacerbating chronic liver inflammation and fibrosis in CLD. MCP-1 may be involved in the monocyte infiltration and progression of liver inflammation and fibrosis in CLD.