ABSTRACT
Proton exchange membrane fuel cells (PEMFCs) and alkaline membrane fuel cells (AEMFCs) have received great attention as energy devices of the next generation. Accelerating oxygen reduction reaction (ORR) kinetics is the key to improve PEMFC and AEMFC performance. Platinum-based catalysts are the most widely used catalysts for the ORR, but their high price and low abundance limit the commercialization of fuel cells. Non-noble metal-nitrogen-carbon (M-N-C) is considered to be the most likely material class to replace Pt-based catalysts, among which Fe-N-C and Co-N-C have been widely studied due to their excellent intrinsic ORR performance and have made great progress in the past decades. With the improvement of synthesis technology and a deeper understanding of the ORR mechanism, some reported Fe-N-C and Co-N-C catalysts have shown excellent ORR activity close to that of commercial Pt/C catalysts. Inspired by the progress, regulation strategies for Fe-N-C and Co-N-C catalysts are summarized in this Review from 5â perspectives: (1)â coordinated atoms, (2)â environmental heteroatoms and defects, (3)â dual-metal active sites, (4)â metal-based particle promoters, and (5)â curved carbon layers. We also make suggestions on some challenges facing Fe-N-C and Co-N-C research.
ABSTRACT
BACKGROUND: Esophageal cancer (ESCA) is a common malignant tumor of the digestive tract, and its poor prognosis is mainly attributed to the occurrence of invasion and metastasis. Z-DNA binding protein 1 (ZBP1), as a mRNA regulatory factor, plays an important role in the occurrence and development of various tumors. However, the role of ZBP1 in ESCA is not yet understood. AIMS: This study aims to explore the expression of ZBP1 in ESCA and its role in the development of ESCA. METHODS: Using bioinformatics analysis and immunohistochemistry staining, we detected the expression of ZBP1 in ESCA and normal tissues. The potential mechanism of ZBP1 in ESCA was analyzed from the aspects of genetic mutations, protein interaction networks, and pathway enrichment. We performed functional experiments in vitro to elucidate the effect of ZBP1 on ESCA cells. RESULTS: ZBP1 was found to be significantly upregulated in ESCA compared to adjacent noncancerous tissues, and its expression is closely related to gender, age, and lymph node metastasis. In ESCA, the genetic variation rate of ZBP1 is 8%, and its expression is positively correlated with immune cell infiltration. The ZBP1 co-expressed gene is mainly involved in processes such as lymph node proliferation and intercellular adhesion. In vitro experiments have confirmed that downregulation of ZBP1 significantly inhibited the proliferation, migration, and invasion of ESCA cells. CONCLUSION: This research proves that downregulation of ZBP1 can inhibit the progression of ESCA. This finding indicates that ZBP1 may be a novel biomarker to improve the diagnosis and treatment of ESCA.
Subject(s)
Esophageal Neoplasms , RNA-Binding Proteins , Humans , Esophageal Neoplasms/genetics , Esophageal Neoplasms/metabolism , Esophageal Neoplasms/pathology , Male , Female , Middle Aged , RNA-Binding Proteins/metabolism , RNA-Binding Proteins/genetics , Cell Proliferation , Cell Line, Tumor , Gene Expression Regulation, Neoplastic , Lymphatic Metastasis , Aged , Up-Regulation , DNA-Binding Proteins/genetics , DNA-Binding Proteins/metabolismABSTRACT
Background: Thyroid carcinoma (THCA) is one of the most commonly diagnosed malignancies. Collagen is the main component in extracellular matrix. Rising studies have determined the oncogenic effect of collagen in cancer progression, which is intriguing to be further explored. Collagen type XXVI alpha 1 chain (COL26A1) is a newly discovered collagen subtype, functions of which still remain poorly demonstrated in THCA. Methods: Based on the transcriptome data from The Cancer Genome Atlas (TCGA) and other public databases, we conducted investigations of COL26A1 in THCA with respects to diagnostic/prognostic prediction, functional characterization, immune infiltration, chemical drug target and non-coding RNA regulatory network. Furthermore, quantitative real-time polymerase chain reaction (qRT-PCR) and western blot were used to verify the expression of COL26A1 in THCA. Results: COL26A1 was significantly upregulated in THCA, and the high COL26A1 expression inferred poor prognosis [hazard ratio (HR) =4.76; 95% confidence interval (CI): 1.36-16.73; P=0.015]. The diagnostic area under the curve (AUC) of COL26A1 achieved 0.736 (95% CI: 0.669-0.802). COL26A1 was also identified as an independent prognostic predictor for THCA (HR =3.928; 95% CI: 3.716-4.151; P<0.001). Besides, logistic regression analysis indicated that age >45 years [odds ratio (OR) =1.532; 95% CI: 1.081-2.176; P=0.017], pathological stage III (OR =2.055; 95% CI: 1.314-3.184; P=0.001), tall cell subtype (OR =5.533; 95% CI: 2.420-14.957; P<0.001), residual tumor R1 (OR =1.844; 95% CI: 1.035-3.365; P=0.041) and extrathyroidal extension (OR =1.800; 95% CI: 1.225-1.660; P=0.003) were risk factors associated with high COL26A1 expression in THCA. Functional characterizations implied that COL26A1 was associated with immunological processes and oncogenic signaling pathways. High COL26A1 expression was accompanied by more abundant infiltration of immune cells and higher stromal/immune score. In addition, most immune checkpoints were significantly positively co-expressed with COL26A1, including PD-1, PD-L1 and CTLA4. Drugs including trichloroethylene, acetamide and thioacetamide etc. that can decrease the expression of COL26A1 were also identified. The predicted long noncoding RNA (lncRNA)-microRNA (miRNA)-COL26A1 regulatory axes were successfully deciphered. qRT-PCR and western blot verified the upregulation of COL26A1 in THCA. Conclusions: Our work has primarily appraised COL26A1 as a promising biomarker for diagnosis/prognosis and immuno/therapeutic target in THCA.
ABSTRACT
Tailoring the near-surface composition of Pt-based alloy can optimize the surface chemical properties of a nanocatalyst and further improve the sluggish H2 electrooxidation performance in an alkaline electrolyte. However, the construction of alloy nanomaterials with a precise near-surface composition and smaller particle size still needs to overcome huge obstacles. Herein, ultra-small PtRu3 binary nanoparticles (<2 nm) evenly distributed on porous carbon (PtRu3 /PC), with different near-surface atomic compositions (Pt-increased and Ru-increased), are successfully synthesized. XPS characterizations and electrochemical test confirm the transformation of a near-surface atomic composition after annealing PtRu3 /PC-300 alloy; when annealing in CO atmosphere, forming the Pt-increased near-surface structure (500 °C), while the Ru-increased near-surface structure appears in an Ar heat treatment process (700 °C). Furthermore, three PtRu3 /PC nanocatalysts all weaken the hydrogen binding strength relative to the Pt/PC. Remarkably, the Ru-increased nanocatalyst exhibits up to 38.8-fold and 9.2-fold HOR improvement in mass activity and exchange current density, compared with the Pt/PC counterpart, respectively. CO-stripping voltammetry tests demonstrate the anti-CO poisoning ability of nanocatalysts, in the sequence of Ru-increased ≥ PtRu3 /PC-300 > Pt-increased > Pt/PC. From the perspective of engineering a near-surface structure, this study may open up a new route for the development of high-efficiency electrocatalysts with a strong electronic effect and oxophilic effect.
ABSTRACT
Driven by the persisting poor understanding of the sluggish kinetics of the hydrogen evolution reaction (HER) on Pt in alkaline media, a direct correlation of the interfacial water structure and activity is still yet to be established. Herein, using Pt and Pt-Ni nanoparticles we first demonstrate a strong dependence of the proton donor structure on the HER activity and pH. The structure of the first layer changes from the proton acceptors to the donors with increasing pH. In the base, the reactivity of the interfacial water varied its structure, and the activation energies of water dissociation increased in the sequence: the dangling O-H bonds < the trihedrally coordinated water < the tetrahedrally coordinated water. Moreover, optimizing the adsorption of H and OH intermediates can re-orientate the interfacial water molecules with their H atoms pointing towards the electrode surface, thereby enhancing the kinetics of HER. Our results clarified the dynamic role of the water structure at the electrode-electrolyte interface during HER and the design of highly efficient HER catalysts.
ABSTRACT
Metal-containing nanoparticles (M-NPs) in metal/nitrogen-doped carbon (M-N-C) catalysts have been considered hostile to the acidic oxygen reduction reaction (ORR). The relation between M-NPs and the active sites of metal coordinated with nitrogen (MNx ) is hard to establish in acid medium owing to the poor stability of M-NPs. Herein, we develop a strategy to successfully construct a new FeCo-N-C catalyst containing highly active M-NPs and MN4 composite sites (M/FeCo-SAs-N-C). Enhanced catalytic activity and stability of M/FeCo-SAs-N-C is shown experimentally. Calculations reveal that there is a strong interaction between M-NPs and FeN4 sites, which can favor ORR by activating the O-O bond, thus facilitating a direct 4 e- process. Those findings firstly shed light on the highly active M-NPs and FeN4 composite sites for catalyzing acid oxygen reduction reaction, and the relevant reaction mechanism is suggested.
ABSTRACT
Electrochemical nitrogen reduction reaction (NRR) has been considered as a promising alternative to the traditional Haber-Bosch process for the preparation of ammonia (NH3) under ambient conditions. The development of cost-effective electrocatalysts with suppressive activity for hydrogen evolution reaction is critical for improving the efficiency of NRR. Herein, oxygen-containing molybdenum carbides (O-MoC) embedded in nitrogen-doped carbon layers (N-doped carbon) can be easily fabricated by pyrolyzing the chelate of dopamine and molybdate. A rate of NH3 formation of 22.5 µg·h-1·mgcat-1 is obtained at -0.35 V versus reversible hydrogen electrode with a high faradaic efficiency of 25.1% in 0.1 mM HCl + 0.5 M Li2SO4. Notably, the synthesized O-MoC@NC-800 also exhibits high selectivity (no formation of hydrazine) and electrochemical stability. The moderate electron structure induced by the interaction between O-MoC and N-doped carbon shells can effectively weaken the activity of hydrogen evolution reaction and increase the faradaic efficiency of NRR. Additionally, by applying the in situ Fourier transform infrared spectroscopy, an associative reaction pathway is proposed on O-MoC@NC-800. This work provides new insights into the rational design of carbon-encapsulated metal nanoparticles as efficient catalysts for NRR at ambient conditions.
ABSTRACT
Bimetallic PtPb nanodendrites with a single-crystalline structure were obtained by a facile one-pot strategy. The as-synthesized dendritic structure was well characterized and the growth mechanism was investigated. PtPb nanodendrites exhibited superior activity (5.1 times higher than commercial Pd black) and strong anti-poisoning ability for electrooxidation of formic acid.
