A Fluorescent Thermometer Based on a Pyrene-Labeled Thermoresponsive Polymer

Thermoresponsive polymers that undergo a solubility transition by variation of the temperature are important materials for the development of ‘smart’ materials. In this contribution we exploit the solubility phase transition of poly(methoxy diethylene glycol methacrylate), which is accompanied by a transition from hydrophilic to hydrophobic, for the development of a fluorescent thermometer. To translate the polymer phase transition into a fluorescent response, the polymer was functionalized with pyrene resulting in a change of the emission based on the microenvironment. This approach led to a soluble polymeric fluorescent thermometer with a temperature range from 11 °C to 21 °C. The polymer phase transition that occurs during sensing is studied in detail by dynamic light scattering

Comparative U, Np and Pu M edge high energy resolution X-ray absorption spectroscopy (HR-XANES) investigations of model and genuine active waste glass

Understanding the long term behavior of vitrified nuclear waste requires a full and detailed characterization of the materials including their characteristics as synthesized and after exposure to groundwater. Genuine radioactive waste glass has a complex chemical composition. Therefore we take a simplified approach by investigating and comparing the oxidation states of U, Pu and Np in high level waste (HLW) glass sampled from the VEK vitrification process (VEK glass) and in model glasses. The model glasses doped with U and Pu have the same borosilicate glass frit composition as the VEK glass, whereas the model glass doped with Np has a base glass composition (R7T7) typically used for vitrification of HLW in France. U/Pu/Np M4/M5 edge high energy resolution X-ray absorption near edge structure (HR-XANES) spectroscopy technique [1] is applied to characterize the An oxidation states in model and genuine VEK HLW glass. The HR-XANES analyses suggest predominant existence of U(VI) and Pu(IV) in the HLW and the model glasses as expected from the oxidative vitrification conditions. Weak changes in U oxidation state as a function of the U loading (1.2 – 5 wt% UO2) are discussed on the basis of U M4 edge HR-XANES and X-ray photoelectron spectroscopy (XPS) results. One significant difference found between the model and the genuine HLW glasses is the strong radiation damage induced in the HLW glass by the soft X-ray beam (position of the U M4 edge: 3.73 keV) which was not observed for the U doped model glasses and the previous L3 edge investigations of the HLW glass sample. The dominant U(VI) oxidation state is reduced almost by 50% to U(IV) within 5 h of measurement. The complex chemical composition of the HLW glass leads to different local U atomic environments compared to the model glass as found by EXAFS investigations. EXAFS results confirm that U in the HLW glass is coordinated by Al/Si neighbors in the second coordination sphere, whereas no neighboring atoms are observed at this distance for the model glass. Differences in results obtained for the Np oxidation state for Np doped asprepared and leached R7T7 borosilicate model glasses and the HLW glass will be presented and discussed

Comparative U, Np and Pu M edge high energy resolution X-ray absorption spectroscopy (HR-XANES) investigations of model and genuine active waste glass

Genuine radioactive glass sampled from the vitrification plant Karlsruhe and actinide doped model 2 glasses  are  investigated  by  U/Pu/Np  M4/M5  high  energy  resolution  X‐ray  absorption near edge structure (HR‐XANES), U L3 EXAFS and XPS spectroscopy techniques to characterize and compare the U, Pu and Np oxidation states and their local atomic environments. The importance of the results will be discussed in terms of the strategy of using simplified simulated waste glasses to understand more complex industrial glass samples. The final goal of these studies is to predict the long term behavior of vitrified nuclear waste stored in a nuclear waste repository. Highly active waste concentrate (HAWC) from nuclear fuel reprocessing is immobilized in borosilicate glass matrices to generate a disposable waste form [1]. Between 2009 and 2010, the vitrification plant Karlsruhe (VEK) was operated for vitrification of liquid process residues left over from operation of the former reprocessing plant Karlsruhe (WAK). About 56 m3 HAWC were processed, resulting in 50 t of waste  glass  [2].  The  long  term  radiotoxicity  of  U,  Np,  Pu  and  other  actinide  elements  (An),  minor constitute of the reprocessed waste, is of great concern in safety assessment studies of nuclear waste repositories. For example, in case of water intrusion and interaction with the glass matrix, corrosion processes will take place which might facilitate the release of radionuclides into the geosphere. The An redox state and bonding characteristics in the glass matrix determine their release mechanisms and retention processes taking place in near and far field of the repository [3]. Understanding the long term behavior of vitrified nuclear waste requires full and detailed characterization of the materials including their characteristics as synthesized and after exposure to  groundwater. Genuine radioactive waste glass has a complex chemical composition. Therefore we take a simplified approach by investigating and comparing the oxidation states of U, Pu and Np in high level waste (HLW) glass sampled from the VEK vitrification process (VEK glass) and in model glasses. The model glasses doped with U and Pu have the same borosilicate glass frit composition as the VEK glass, whereas  the  model  glass  doped  with  Np  has  a  base  glass  composition  (R7T7)  typically  used  for  vitrification of HLW in France. U/Pu/Np  M4/M5  edge  high  energy  resolution  X‐ray  absorption  near  edge  structure  (HR‐XANES)  spectroscopy technique [4] is applied to characterize the An oxidation states

Introduction to the Conceptualisation of Environmental Citizenship for Twenty-First-Century Education

The EU’s growth strategy (Europe 2020) and the European vision for green, circular and low-carbon economy in line with the EU 2050 (EU-roadmap 2050) give par- ticular attention to citizens’ participation and engagement and therefore to Environmental Citizenship. Environmental Citizenship has been an influential con- cept in many different arenas such as economy, policy, philosophy, corporation management and marketing, which could also be better exploited and established in the field of education. Environmental Citizenship is recognized as an important aspect in addressing global environmental problems such as climate change (Stern 2011; Ockwell et al. 2009) whilst providing support to pro-environmental organisa- tions and individuals, contributing also to public pressure for political action (sign- ing petitions, writing to politicians and newspapers). Many varied definitions of Environmental Citizenship can be found within the literature. Some of them are quite similar, and important overlaps can be observed; however, others can be quite different with contradictions in their philosophy and approach. According to Dobson (2010), Environmental Citizenship refers to pro-environmental behaviour, in public and in private, driven by a belief in fairness of the distribution of environmental goods, in participation and in the co-creation of sustainability policy. It is about the active participation of citizens in moving towards sustainability. Education and especially environmental discourses in science education have a lot to contribute in adopting and promoting Environmental Citizenship. However, the conceptualisation of Environmental Citizenship in educational context remains an imperative need. The under-explored (until now) potential for pro-environmental behaviour change through Environmental Citizenship should be further emphasised (Dobson 2010) and can contribute greatly to a more sustainable world.info:eu-repo/semantics/publishedVersio

The iBeetle large-scale RNAi screen reveals gene functions for insect development and physiology

Genetic screens are powerful tools to identify the genes required for a given biological process. However, for technical reasons, comprehensive screens have been restricted to very few model organisms. Therefore, although deep sequencing is revealing the genes of ever more insect species, the functional studies predominantly focus on candidate genes previously identified in Drosophila, which is biasing research towards conserved gene functions. RNAi screens in other organisms promise to reduce this bias. Here we present the results of the iBeetle screen, a large-scale, unbiased RNAi screen in the red flour beetle, Tribolium castaneum, which identifies gene functions in embryonic and postembryonic development, physiology and cell biology. The utility of Tribolium as a screening platform is demonstrated by the identification of genes involved in insect epithelial adhesion. This work transcends the restrictions of the candidate gene approach and opens fields of research not accessible in Drosophila

Computational Identification of Transcriptional Regulators in Human Endotoxemia

One of the great challenges in the post-genomic era is to decipher the underlying principles governing the dynamics of biological responses. As modulating gene expression levels is among the key regulatory responses of an organism to changes in its environment, identifying biologically relevant transcriptional regulators and their putative regulatory interactions with target genes is an essential step towards studying the complex dynamics of transcriptional regulation. We present an analysis that integrates various computational and biological aspects to explore the transcriptional regulation of systemic inflammatory responses through a human endotoxemia model. Given a high-dimensional transcriptional profiling dataset from human blood leukocytes, an elementary set of temporal dynamic responses which capture the essence of a pro-inflammatory phase, a counter-regulatory response and a dysregulation in leukocyte bioenergetics has been extracted. Upon identification of these expression patterns, fourteen inflammation-specific gene batteries that represent groups of hypothetically ‘coregulated’ genes are proposed. Subsequently, statistically significant cis-regulatory modules (CRMs) are identified and decomposed into a list of critical transcription factors (34) that are validated largely on primary literature. Finally, our analysis further allows for the construction of a dynamic representation of the temporal transcriptional regulatory program across the host, deciphering possible combinatorial interactions among factors under which they might be active. Although much remains to be explored, this study has computationally identified key transcription factors and proposed a putative time-dependent transcriptional regulatory program associated with critical transcriptional inflammatory responses. These results provide a solid foundation for future investigations to elucidate the underlying transcriptional regulatory mechanisms under the host inflammatory response. Also, the assumption that coexpressed genes that are functionally relevant are more likely to share some common transcriptional regulatory mechanism seems to be promising, making the proposed framework become essential in unravelling context-specific transcriptional regulatory interactions underlying diverse mammalian biological processes

Induction of effective and antigen-specific antitumour immunity by a liposomal ErbB2/HER2 peptide-based vaccination construct

Efficient delivery of tumour-associated antigens to appropriate cellular compartments of antigen-presenting cells is of prime importance for the induction of potent, cell-mediated antitumour immune responses. We have designed novel multivalent liposomal constructs that co-deliver the p63–71 cytotoxic T Lymphocyte epitope derived from human ErbB2 (HER2), and HA307–319, a T-helper (Th) epitope derived from influenza haemagglutinin. Both peptides were conjugated to the surface of liposomes via a Pam3CSS anchor, a synthetic lipopeptide with potent adjuvant activity. In a murine model system, vaccination with these constructs completely protected BALB/c mice from subsequent s.c. challenge with ErbB2-expressing, but not ErbB2-negative, murine renal carcinoma (Renca) cells, indicating the induction of potent, antigen-specific immune responses. I.v. re-challenge of tumour-free animals 2 months after the first tumour cell inoculation did not result in the formation of lung tumour nodules, suggesting that long-lasting, systemic immunity had been induced. While still protecting the majority of vaccinated mice, a liposomal construct lacking the Th epitope was less effective than the diepitope construct, also correlating with a lower number of CD8+ IFN-γ+ T-cells identified upon ex vivo peptide restimulation of splenocytes from vaccinated animals. Importantly, in a therapeutic setting treatment with the liposomal vaccines resulted in cures in the majority of tumour-bearing mice and delayed tumour growth in the remaining ones. Our results demonstrate that liposomal constructs which combine Tc and Th peptide antigens and lipopeptide adjuvants can induce efficient, antigen-specific antitumour immunity, and represent promising synthetic delivery systems for the design of specific antitumour vaccines

The Concise Guide to PHARMACOLOGY 2013/14: overview.

The Concise Guide to PHARMACOLOGY 2013/14 provides concise overviews of the key properties of over 2000 human drug targets with their pharmacology, plus links to an open access knowledgebase of drug targets and their ligands (www.guidetopharmacology.org), which provides more detailed views of target and ligand properties from the IUPHAR database. The full contents can be found at http://onlinelibrary.wiley.com/doi/10.1111/bph.12444/full. This compilation of the major pharmacological targets is divided into seven areas of focus: G protein-coupled receptors, ligand-gated ion channels, ion channels, catalytic receptors, nuclear hormone receptors, transporters and enzymes. These are presented with nomenclature guidance and summary information on the best available pharmacological tools, alongside key references and suggestions for further reading. A new landscape format has easy to use tables comparing related targets. It is a condensed version of material contemporary to late 2013, which is presented in greater detail and constantly updated on the website www.guidetopharmacology.org, superseding data presented in previous Guides to Receptors & Channels. It is produced in conjunction with NC-IUPHAR and provides the official IUPHAR classification and nomenclature for human drug targets, where appropriate. It consolidates information previously curated and displayed separately in IUPHAR-DB and GRAC and provides a permanent, citable, point-in-time record that will survive database updates