Rapid One-Step Capturing of Native, Cell-Free Synthesized and Membrane-Embedded GLP-1R

G protein-coupled receptors (GPCRs) are of outstanding pharmacological interest as they are abundant in cell membranes where they perform diverse functions that are closely related to the vitality of cells. The analysis of GPCRs in natural membranes is laborious, as established methods are almost exclusively cell culture-based and only a few methods for immobilization in a natural membrane outside the cell are known. Within this study, we present a one-step, fast and robust immobilization strategy of the GPCR glucagon-like peptide 1 receptor (GLP-1R). GLP-1R was synthesized in eukaryotic lysates harboring endogenous endoplasmic reticulum-derived microsomes enabling the embedment of GLP-1R in a natural membrane. Interestingly, we found that these microsomes spontaneously adsorbed to magnetic Neutravidin beads thus providing immobilized membrane protein preparations which required no additional manipulation of the target receptor or its supporting membrane. The accessibility of the extracellular domain of membrane-embedded and bead-immobilized GLP-1R was demonstrated by bead-based enzyme-linked immunosorbent assay (ELISA) using GLP-1R-specific monoclonal antibodies. In addition, ligand binding of immobilized GLP-1R was verified in a radioligand binding assay. In summary, we present an easy and straightforward synthesis and immobilization methodology of an active GPCR which can be beneficial for studying membrane proteins in general

Early release of H2O during subduction of carbonated ultramafic lithologies

To investigate the effect of carbon-bearing phases on the release of fluids in subducted serpentinites, we performed high-pressure multi-anvil experiments on representative ophicarbonate assemblages over a pressure range from 2.5 GPa to 5 GPa and from 450 °C to 900 °C, across the antigorite-out reaction. Parallel experiments were performed on carbonate-free serpentinites. In all experiments, we monitored and/or controlled the oxygen fugacity. The addition of 20 wt. % CaCO3 to a serpentinite assemblage at 2.5 GPa is found to decrease the onset of the serpentine dehydration by over 100 °C, in comparison to carbonate-free assemblages. Similarly, the final disappearance of serpentine is also affected by the presence of CaCO3. For a bulk CaCO3 content of 20 wt. %, this causes a decrease in maximum stability of antigorite by 50 °C. For a bulk CaCO3 content exceeding 25 wt. %, this difference can be as high as 100 °C in warm and 150 °C in cold subduction zones, causing antigorite to be completely dehydrated at 500 °C. This results from the reaction of CaCO3 with serpentine to form clinopyroxene and Mg-rich carbonates. This reaction, however, causes no discernible decrease in the proportion of carbonate, indicating that the amount of released carbon is insignificant. Whilst CaCO3, therefore, influences serpentine stability, there is no significant effect of hydrous phases on the carbonate stability. On the other hand, a MgCO3-bearing system shows no significant effects on the serpentinite stability field. Further experiments and oxygen fugacity calculations indicate that graphite is not stable in typical magnetite-bearing serpentinites. The reduction of carbonates to graphite would require oxygen fugacities that are 1–2 log units below those of magnetite-bearing serpentinites. This confirms earlier studies and indicates that reduction of carbonates can only occur through the infiltration of external H2-rich fluids

Tumor Cell-Based Vaccine Generated With High Hydrostatic Pressure Synergizes With Radiotherapy by Generating a Favorable Anti-tumor Immune Microenvironment

Dendritic cell (DC)-based vaccines pulsed with high hydrostatic pressure (HHP)-inactivated tumor cells have been demonstrated to be a promising immunotherapy for solid tumors. We focused on sole injection of tumor cells that were inactivated by HHP and their combination with local radiotherapy (RTx) for in vivo induction of anti-tumor immune responses. HHP-treatment of tumor cells resulted in pre-dominantly necrotic cells with degraded DNA. We confirmed that treatments at 200 MPa or higher completely inhibited the formation of tumor cell colonies in vitro. No tumor growth was seen in vivo after injection of HHP-treated tumor cells. Single vaccination with HHP-killed tumor cells combined with local RTx significantly retarded tumor growth and improved the survival as shown in B16-F10 and CT26 tumor models. In B16-F10 tumors that were irradiated with 2 × 5Gy and vaccinated once with HHP-killed tumor cells, the amount of natural killer (NK) cells, monocytes/macrophages, CD4+ T cells and NKT cells was significantly increased, while the amount of B cells was significantly decreased. In both models, a trend of increased CD8+ T cell infiltration was observed. Generally, in irradiated tumors high amounts of CD4+ and CD8+ T cells expressing PD-1 were found. We conclude that HHP generates inactivated tumor cells that can be used as a tumor vaccine. Moreover, we show for the first time that tumor cell-based vaccine acts synergistically with RTx to significantly retard tumor growth by generating a favorable anti-tumor immune microenvironment

Criteria for the use of omics-based predictors in clinical trials.

The US National Cancer Institute (NCI), in collaboration with scientists representing multiple areas of expertise relevant to 'omics'-based test development, has developed a checklist of criteria that can be used to determine the readiness of omics-based tests for guiding patient care in clinical trials. The checklist criteria cover issues relating to specimens, assays, mathematical modelling, clinical trial design, and ethical, legal and regulatory aspects. Funding bodies and journals are encouraged to consider the checklist, which they may find useful for assessing study quality and evidence strength. The checklist will be used to evaluate proposals for NCI-sponsored clinical trials in which omics tests will be used to guide therapy

Development of a GEM-TPC prototype

The use of GEM foils for the amplification stage of a TPC instead of a con- ventional MWPC allows one to bypass the necessity of gating, as the backdrift is suppressed thanks to the asymmetric field configuration. This way, a novel continuously running TPC, which represents one option for the PANDA central tracker, can be realized. A medium sized prototype with a diameter of 300 mm and a length of 600 mm will be tested inside the FOPI spectrometer at GSI using a carbon or lithium beam at intermediate energies (E = 1-3AGeV). This detector test under realistic experimental conditions should allow us to verify the spatial resolution for single tracks and the reconstruction capability for displaced vertexes. A series of physics measurement implying pion beams is scheduled with the FOPI spectrometer together with the GEM-TPC as well.Comment: 5 pages, 4 figures, Proceedings for 11th ICATTP conference in como (italy

Satori 2017

The Satori is a student literary publication that expresses the artistic spirit of the students of Winona State University. Student poetry, prose, and graphic art are published in the Satori every spring since 1970. The Satori 2017 editors are: Editor-in-Chief: Sajda Omar Poetry Editor: Karl Hanson Art/Design Editor: Danielle Eberhard Prose Editor: Cassie Douglas Poetry Committee: Kelly Johnson and Lydia Papenfuss Art/Design Committee: Aurie Brighton and Xinyue Wang Prose Committee: Katie McCoy, Madison Wilke, Megan Back, Alayna Godfrey, Madelyn Hall, and Sam Stormoen Faculty Advisor: Dr. Gary Eddy, Professor of Englishhttps://openriver.winona.edu/satori/1013/thumbnail.jp