Composite nanostructured solid-acid fuel-cell electrodes via electrospray deposition

Stable, porous, nanostructured composite electrodes were successfully fabricated via the inexpensive and scalable method of electrospray deposition, in which a dissolved solute is deposited onto a substrate using an electric field to drive droplet migration. The desirable characteristics of high porosity and high surface area were obtained under conditions that favored complete solvent evaporation from the electrospray droplets prior to contact with the substrate. Solid acid (CsH_2PO_4) feature sizes of 100 nm were obtained from electrosprayed water–methanol solutions with 10 g L^(−1) CsH_2PO_4 and 5 g L^(−1) Pt catalyst particles suspended using polyvinylpyrrolidone (PVP). Alternative additives such as Pt on carbon and carbon-nanotubes (CNTs) were also successfully incorporated by this route, and in all cases the PVP could be removed from the electrode by oxygen plasma treatment without damage to the structure. In the absence of additives (Pt, Pt/C and CNTs), the feature sizes were larger, 300 nm, and the structure morphologically unstable, with significant coarsening evident after exposure to ambient conditions for just two days. Electrochemical impedance spectroscopy under humidified hydrogen at 240 °C indicated an interfacial impedance of ~1.5 Ω cm^2 for the Pt/CsH_2PO_4 composite electrodes with a total Pt loading of 0.3 ± 0.2 mg cm^(−2). This result corresponds to a 30-fold decrease in Pt loading relative to mechanically milled electrodes with comparable activity, but further increases in activity and Pt utilization are required if solid acid fuel cells are to attain widespread commercial adoption

Taking an Active role in an International Project: A Report of a Collaborative Research with Teacher Trainees in UK, Norway and Pakistan

This report introduces an innovative research project about the dialogue among teacher trainees from UK, Norway and Pakistan, about a literary work, in a virtual environment. This project involved us, five English in Education academics from the three contexts, as researchers who gathered, analysed and reported on the international data collaboratively. We reflect on our experience as international researchers and the benefits we found in this type of association across borders for future teachers. This work has implications for teacher education and the methodologies used can be beneficial for future researchers and teacher educators

SWI/SNF-like chromatin remodeling factor Fun30 supports point centromere function in S. cerevisiae

Budding yeast centromeres are sequence-defined point centromeres and are, unlike in many other organisms, not embedded in heterochromatin. Here we show that Fun30, a poorly understood SWI/SNF-like chromatin remodeling factor conserved in humans, promotes point centromere function through the formation of correct chromatin architecture at centromeres. Our determination of the genome-wide binding and nucleosome positioning properties of Fun30 shows that this enzyme is consistently enriched over centromeres and that a majority of CENs show Fun30-dependent changes in flanking nucleosome position and/or CEN core micrococcal nuclease accessibility. Fun30 deletion leads to defects in histone variant Htz1 occupancy genome-wide, including at and around most centromeres. FUN30 genetically interacts with CSE4, coding for the centromere-specific variant of histone H3, and counteracts the detrimental effect of transcription through centromeres on chromosome segregation and suppresses transcriptional noise over centromere CEN3. Previous work has shown a requirement for fission yeast and mammalian homologs of Fun30 in heterochromatin assembly. As centromeres in budding yeast are not embedded in heterochromatin, our findings indicate a direct role of Fun30 in centromere chromatin by promoting correct chromatin architecture

Kinesins relocalize the chromosomal passenger complex to the midzone for spindle disassembly.

Mitotic spindle disassembly after chromosome separation is as important as spindle assembly, yet the molecular mechanisms for spindle disassembly are unclear. In this study, we investigated how the chromosomal passenger complex (CPC), which contains the Aurora B kinase Ipl1, swiftly concentrates at the spindle midzone in late anaphase, and we researched the role of this dramatic relocalization during spindle disassembly. We showed that the kinesins Kip1 and Kip3 are essential for CPC relocalization. In cells lacking Kip1 and Kip3, spindle disassembly is severely delayed until after contraction of the cytokinetic ring. Purified Kip1 and Kip3 interact directly with the CPC and recruit it to microtubules in vitro, and single-molecule experiments showed that the CPC diffuses dynamically on microtubules but that diffusion stops when the CPC encounters a Kip1 molecule. We propose that Kip1 and Kip3 trap the CPC at the spindle midzone in late anaphase to ensure timely spindle disassembly