Regulation of Electrocatalytic Activity by Local Microstructure: Focusing on the Catalytic Active Zone.

Traditional regulation methods of active sites have successfully optimized the performance of electrocatalysts, but seem unable to achieve further breakthrough in the catalytic activity. Unlike the conventional viewpoint of focusing on single active site, the concept of local microstructure active zone is more comprehensive and new methods to regulate the reaction zone for electrocatalytic reactions are developed accordingly. The local microstructure active zone refers to the zone with high catalytic activity formed by the interaction between active atoms and neighboring coordination atoms as well as the surrounding environment. Instead of the traditional single active atom site, the active zone is more suitable for the actual electrochemical reaction process. According to this concept, the activity of electrocatalysts can be coordinated by multiple active atoms. This strategy is beneficial for understanding the relationship between material, structure, and catalysis, which realizes the design and synthesis of high-performance electrocatalysts. This review provides the research progress of this strategy for electrocatalytic reactions, with emphasis on their applications in oxygen evolution reaction, urea oxidation reaction, and carbon dioxide reduction.

FeCo Nanoparticles Encapsulated in N-Doped Carbon Nanotubes Coupled with Layered Double (Co, Fe) Hydroxide as an Efficient Bifunctional Catalyst for Rechargeable Zinc-Air Batteries.

Low-cost bifunctional nonprecious metal catalysts toward oxygen reduction reaction (ORR) and oxygen evolution reaction (OER) are critical for the commercialization of rechargeable zinc-air batteries (ZABs). However, the preparation of highly active and durable bifunctional catalysts is still challenging. Herein, an efficient catalyst is reported consisting of FeCo nanoparticles embedded in N-doped carbon nanotubes (FeCo NPs-N-CNTs) by an in situ catalytic strategy. Due to the encapsulation and porous structure of N-doped carbon nanotubes, the catalyst shows high activity toward ORR and excellent durability. Furthermore, to enhance the OER activity, CoFe-layer double hydroxide (CoFe-LDH) is coupled with FeCo NPs-N-CNTs by in situ reaction approach. As the air electrode for rechargeable ZABs, the cell with CoFe-LDH@FeCo NPs-N-CNTs catalyst exhibits high open-circuit potential (OCP) of 1.51 V, high power density of 116 mW cm-2 , and remarkable durability up to 100 h, demonstrating its great promise for the practical application of the rechargeable ZABs.

Oxygen Deficient LaMn0.75Co0.25O3-δ Nanofibers as an Efficient Electrocatalyst for Oxygen Evolution Reaction and Zinc-Air Batteries.

The rational design of efficient and durable oxygen evolution reaction (OER) is important for energy conversion and storage devices. Here, we develop a two-step calcination method to prepare cobalt nanoparticles uniformly dispersed on perovskite oxide nanofibers and to tune oxygen vacancies in perovskite LaMn0.75Co0.25O3-δ nanofibers. The obtained product shows enhanced activity toward OER. In particular, the oxygen deficient LMCO-2 catalyst prepared by a two-step calcination shows excellent OER performance that is 27.5 times that of the LMO catalyst and is comparable to that of the commercial RuO2 catalyst. It also demonstates good stability because of its novel structure, abundant oxygen vacancies, and larger number of metal ions with a high oxidation state. As an air electrode for a flexible zinc-air battery, the cell with the LMCO-2 catalyst delivers a higher power density of 35 mW cm-2 and excellent cycling stability for 70 h. Moreover, the cell exhibits excellent flexibility under different bending conditions.

Multistep Dissolution of Lamellar Crystals Generates Superthin Amorphous Ni(OH)2 Catalyst for UOR.

Urea oxidation reaction (UOR) is an ideal replacement of the conventional anodic oxygen evolution reaction (OER) for efficient hydrogen production due to the favorable thermodynamics. However, the UOR activity is severely limited by the high oxidation potential of Ni-based catalysts to form Ni3+ , which is considered as the active site for UOR. Herein, by using in situ cryoTEM, cryo-electron tomography, and in situ Raman, combined with theoretical calculations, a multistep dissolution process of nickel molybdate hydrate is reported, whereby NiMoO4 ·xH2 O nanosheets exfoliate from the bulk NiMoO4 ·H2 O nanorods due to the dissolution of Mo species and crystalline water, and further dissolution results in superthin and amorphous nickel (II) hydroxide (ANH) flocculus catalyst. Owing to the superthin and amorphous structure, the ANH catalyst can be oxidized to NiOOH at a much lower potential than conventional Ni(OH)2 and finally exhibits more than an order of magnitude higher current density (640 mA cm-2 ), 30 times higher mass activity, 27 times higher TOF than those of Ni(OH)2 catalyst. The multistep dissolution mechanism provides an effective methodology for the preparation of highly active amorphous catalysts.

Recent Advances in Single-Atom Electrocatalysts for Oxygen Reduction Reaction.

Oxygen reduction reaction (ORR) plays significant roles in electrochemical energy storage and conversion systems as well as clean synthesis of fine chemicals. However, the ORR process shows sluggish kinetics and requires platinum-group noble metal catalysts to accelerate the reaction. The high cost, rare reservation, and unsatisfied durability significantly impede large-scale commercialization of platinum-based catalysts. Single-atom electrocatalysts (SAECs) featuring with well-defined structure, high intrinsic activity, and maximum atom efficiency have emerged as a novel field in electrocatalytic science since it is promising to substitute expensive platinum-group noble metal catalysts. However, finely fabricating SAECs with uniform and highly dense active sites, fully maximizing the utilization efficiency of active sites, and maintaining the atomically isolated sites as single-atom centers under harsh electrocatalytic conditions remain urgent challenges. In this review, we summarized recent advances of SAECs in synthesis, characterization, oxygen reduction reaction (ORR) performance, and applications in ORR-related H2O2 production, metal-air batteries, and low-temperature fuel cells. Relevant progress on tailoring the coordination structure of isolated metal centers by doping other metals or ligands, enriching the concentration of single-atom sites by increasing metal loadings, and engineering the porosity and electronic structure of the support by optimizing the mass and electron transport are also reviewed. Moreover, general strategies to synthesize SAECs with high metal loadings on practical scale are highlighted, the deep learning algorithm for rational design of SAECs is introduced, and theoretical understanding of active-site structures of SAECs is discussed as well. Perspectives on future directions and remaining challenges of SAECs are presented.

One-trial in vitro conditioning of hermissenda regulates phosphorylation of ser-122 of csp24.

The regulation of the intrinsic excitability of a neuron is an important aspect of cellular and synaptic plasticity underlying learning and memory. Various voltage-dependent K(+) channels have been shown to be critical for the modification of membrane excitability. Components of the cytoskeleton have been proposed to contribute to the location, distribution, and function of diverse K(+) channels. However, the mechanisms underlying the regulation of the cytoskeleton by signaling pathways and the role of the cytoskeleton in the induction of intrinsic excitability is not understood. Hermissenda Csp24 is a beta-thymosin-like protein containing multiple actin-binding domains that contributes to intrinsic enhanced excitability produced by Pavlovian conditioning. One-trial in vitro conditioning produces a significant reduction in the A-type transient K(+) current (I(A)) and a depolarized shift in the steady-state activation curve of I(A). Intermediate and long-term enhanced excitability produced by one-trial conditioning is also dependent on the expression and phosphorylation of Csp24. Blocking the expression of Csp24 with an antisense oligonucleotide inhibits the development of intermediate-term enhanced excitability and the concomitant reduction in I(A) normally produced by one-trial in vitro conditioning. In this report using two-dimensional gel PAGE and electrospray mass spectrometry, we have identified two phosphorylation sites on Csp24. Using phospho-specific antibodies with Western blot analysis and immunoprecipitation procedures we show that one-trial in vitro conditioning results in an increase in the phosphorylation of Ser-122, but not Ser-49 of Csp24.

14-3-3 proteins interact with the beta-thymosin repeat protein Csp24.

Conditioned stimulus pathway protein 24 (Csp24) is a beta-thymosin-like protein that is homologous to other members of the family of beta-thymosin repeat proteins that contain multiple actin binding domains. Actin co-precipitates with Csp24 and co-localizes with it in the cytosol of type-B photoreceptor cell bodies. Several signal transduction pathways have been shown to regulate the phosphorylation of Csp24 and contribute to cellular plasticity. Here, we report the identification of the adapter protein 14-3-3 in lysates of the Hermissenda circumesophageal nervous system and its interaction with Csp24. Immunoprecipitation experiments using an antibody that is broadly reactive with several isoforms of the 14-3-3 family of proteins showed that Csp24 co-precipitates with 14-3-3 protein, and nervous systems stimulated with 5-HT exhibited a significant increase in co-precipitated Csp24 probed with a phosphospecific antibody as compared with controls. These results indicate that post-translational modifications of Csp24 regulate its interaction with 14-3-3 protein, and suggest that this mechanism may contribute to the control of intrinsic enhanced excitability.

Rho/ROCK and Cdk5 effects on phosphorylation of a beta-thymosin repeat protein in Hermissenda.

Rho GTPases acting through effector proteins regulate actin dynamics and cytoskeletal structure. In Hermissenda Csp24 is a cytoskeletal-related protein that contributes to the development of intermediate-term memory, and is homologous to other beta-thymosin-like repeat proteins containing multiple actin-binding domains. We have examined the role of Rho GTPase activity and its downstream target ROCK, and cyclin-dependent kinase 5 (Cdk5) on the phosphorylation of Csp24 using 32PO4 labeling of proteins separated with 2-D PAGE. The ROCK inhibitor Y-27632 significantly increased Csp24 phosphorylation, and the Rho activator lysophosphatidic acid (LPA) or the Cdk5 inhibitor butyrolactone significantly decreased Csp24 phosphorylation. Pretreatment with Y-27632 before LPA application significantly reduced the decreased phosphorylation of Csp24 normally detected in nervous systems exposed to LPA. Using a pull-down assay we found that LPA treatments activated Rho and exposure to 5-HT decreased Rho activity. Our results indicate that the Rho/ROCK and Cdk5 signaling pathways contribute to the regulation of Csp24 phosphorylation.