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Models propose an auditory-motor mapping via a left-hemispheric dorsal speech-processing stream, yet its detailed contributions to speech perception and production are unclear. Using fMRI-navigated repetitive transcranial magnetic stimulation (rTMS), we virtually lesioned left dorsal stream components in healthy human subjects and probed the consequences on speech-related facilitation of articulatory motor cortex (M1) excitability, as indexed by increases in motor-evoked potential (MEP) amplitude of a lip muscle, and on speech processing performance in phonological tests. Speech-related MEP facilitation was disrupted by rTMS of the posterior superior temporal sulcus (pSTS), the sylvian parieto-temporal region (SPT), and by double-knock-out but not individual lesioning of pars opercularis of the inferior frontal gyrus (pIFG) and the dorsal premotor cortex (dPMC), and not by rTMS of the ventral speech-processing stream or an occipital control site. RTMS of the dorsal stream but not of the ventral stream or the occipital control site caused deficits specifically in the processing of fast transients of the acoustic speech signal. Performance of syllable and pseudoword repetition correlated with speech-related MEP facilitation, and this relation was abolished with rTMS of pSTS, SPT, and pIFG. Findings provide direct evidence that auditory-motor mapping in the left dorsal stream causes reliable and specific speech-related MEP facilitation in left articulatory M1. The left dorsal stream targets the articulatory M1 through pSTS and SPT constituting essential posterior input regions and parallel via frontal pathways through pIFG and dPMC. Finally, engagement of the left dorsal stream is necessary for processing of fast transients in the auditory signal.
Photorhabdus are highly effective insect pathogenic bacteria that exist in a mutualistic relationship with Heterorhabditid nematodes. Unlike other members of the genus, Photorhabdus asymbiotica can also infect humans. Most Photorhabdus cannot replicate above 34°C, limiting their host-range to poikilothermic invertebrates. In contrast, P. asymbiotica must necessarily be able to replicate at 37°C or above. Many well-studied mammalian pathogens use the elevated temperature of their host as a signal to regulate the necessary changes in gene expression required for infection. Here we use RNA-seq, proteomics and phenotype microarrays to examine temperature dependent differences in transcription, translation and phenotype of P. asymbiotica at 28°C versus 37°C, relevant to the insect or human hosts respectively. Our findings reveal relatively few temperature dependant differences in gene expression. There is however a striking difference in metabolism at 37°C, with a significant reduction in the range of carbon and nitrogen sources that otherwise support respiration at 28°C. We propose that the key adaptation that enables P. asymbiotica to infect humans is to aggressively acquire amino acids, peptides and other nutrients from the human host, employing a so called “nutritional virulence” strategy. This would simultaneously cripple the host immune response while providing nutrients sufficient for reproduction. This might explain the severity of ulcerated lesions observed in clinical cases of Photorhabdosis. Furthermore, while P. asymbiotica can invade mammalian cells they must also resist immediate killing by humoral immunity components in serum. We observed an increase in the production of the insect Phenol-oxidase inhibitor Rhabduscin normally deployed to inhibit the melanisation immune cascade. Crucially we demonstrated this molecule also facilitates protection against killing by the alternative human complement pathway.
Pharmakophore sind ein zentrales Konzept der medizinischen Chemie. Im Liganden-basierten Design abstrahieren sie physikochemische Eigenschaften einer Menge aktiver Liganden und lassen dadurch Rückschlüsse auf die möglichen Interaktionen mit einem Target zu. Umgekehrt werden im Struktur-basierten Design Kristallstrukturen von Proteinen genutzt um zu modellieren, welche Eigenschaften die Bindetasche besitzt und welche Eigenschaften das entsprechende Gegenstück möglicher Liganden habe sollte. Diese Informationen können genutzt werden, um neue Substanzen zu identifizieren, welche die im Pharmakophore-Modell modellierten Interaktionen mit dem Target eingehen können. Durch die Abstraktion können hierbei sowohl Verbindungen mit neuen Grundgerüsten (scaffold) als auch mit veränderten funktionellen Gruppen gefunden werden. Im ersten Fall spricht man dabei von „scaffold hopping“, der letzte Fall ist eng verbunden mit dem Konzept des bioisosteren Ersatzes.
Im Rahmen dieser Arbeit wurden Pharmakophore genutzt, um in drei Studien neue Inhibitoren der Arachidonsäurekaskade zu finden. Die Arachidonsäurekaskade ist ein Stoffwechselweg in der aus Arachidonsäure eine Reihe von Lipidmediatoren synthetisiert wird. Viele dieser Mediatoren spielen eine entscheidende Rolle in Entzündungsprozessen und damit einhergehenden Krankheitsbildern. Es wurde außerdem eine neue Methode zur automatischen Generierung von Pharmakophor-Modellen aus einer Menge bekannter Liganden entwickelt.
In der ersten Studie wurde ein Struktur-basiertes Pharmakophor-Modell der Bindetasche der löslichen Epoxidhydrolase (sEH) erstellt, welches die möglichen, relevanten Interaktionsmöglichkeiten abbilden sollte. Dieses Pharmakophor-Modell wurde zum Screening einer Datenbank kommerziell erhältlicher Verbindungen genutzt und führte zu zwei Verbindungen mit IC50-Werten im niedrigen mikromolaren Bereich sowie einer dritten Verbindung mit einem bisher nicht für Inhibitoren der sEH beschriebenem Chemotyp. Zwar war diese Verbindung in höheren Konzentration unlöslich war, jedoch erreichten Derivate ebenfalls IC50-Werte im niedrigen mikromolaren Bereich und könnten als mögliche Startpunkte für eine neue Substanzklasse von sEH-Inhibitoren dienen.
In einer zweiten Studie wurde ein Liganden-basierter Ansatz gewählt um neue Inhibitoren der Leukotrien-A4 Hydrolase (LTA4H) zu suchen. Im Rahmen dieser Studie wurde außerdem eine neue Methode zur automatischen Generierung von Pharmakophor-Modellen entwickelt, welche auf einem wachsenden neuronalen Gas basiert, einer Methode aus dem Bereich des maschinellen Lernens. Die Methode wurde retrospektiv anhand mehrerer Benchmark-Datensätze validiert. Unter anderem wurde überprüft, inwiefern die Methode in der Lage ist die bioaktive Konformation eines Liganden vorherzusagen. Hierzu wurden, ausgehend von co-kristallisierten Liganden, automatisch Modelle generiert, welche im Anschluss genutzt wurden um Konformations-Datenbanken der Liganden zu durchsuchen. Je näher die beste gefundene Konformation an der co-kristallisierten Konformation lag, desto besser war das erzeugte Modell. Die entwickelte Methode war in nahezu allen Fällen in der Lage ein Modell zu erzeugen, mit welchem die durchschnittliche Abweichung zwischen co-kristallisierter und gefundener Konformation unter 2 Å lag. Im Rahmen der Studie wurde die neu entwickelte Methode auch in einem prospektiven Virtual Screening nach neuen Liganden der LTA4H genutzt. Hierzu wurden basierend auf 24 Kristallstrukturen mehrere Pharmakophor-Modelle für LTA4H-Liganden erstellt. Durch zusätzliche Nutzung des ESshape3D Fingerprints konnte außerdem die Form der Bindetasche der LTA4H erfasst werden. Diese Modelle wurden anschließend eingesetzt um eine Datenbank kommerziell erhältlicher Verbindungen zu durchsuchen und führten zur Identifizierung von zwei Substanzen mit IC50-Werten im unteren mikromolaren Bereich. Des Weiteren war die neue Methode in der Lage, den Bindemodus des genutzten Referenzinhibitors vorherzusagen, welcher durch Röntgenstrukturanalyse bestätigt wurde.
In zwei weiteren Studien wurde versucht, duale Inhibitoren der sEH und der 5-Lipoxygenase (5-LO) zu finden. Die erste dieser beiden Studien nutzte hierfür „duale“ Pharmakophor-Modelle: für beide Targets wurde basierend auf einer Vielzahl publizierter, aktiver Liganden eine Reihe von Pharmakophor-Modellen erstellt. Diese Modelle wurden paarweise miteinander verglichen; Modelle, welche eine ausreichend hohe Überlappung an Features besaßen, dienten als Ausgangspunkt für die Suche nach potentiell dualen Liganden. Durch die Suche in einer Fragment-Datenbank konnten neun Verbindungen identifiziert werden, welche eine Aktivität gegenüber einem der beiden Targets zeigten. Diese Verbindungen besaßen zum Teil noch nicht in der Literatur für sEH- oder 5 LO Inhibitoren beschriebene Strukturmerkmale. Eine der Verbindungen war außerdem in der Lage beide Targets im niedrigen mikromolaren Bereich zu inhibieren und könnte als Ausgangspunkt zur Entwicklung weiterer dualer 5-LO/sEH-Inhibitoren dienen. In der zweiten Studie wurde eine auf selbst-organisierenden Karten (SOM) basierende Methode genutzt um potentiell duale Liganden zu suchen. Hierzu wird je eine SOM mit repräsentativen (Sub-) Strukturen von Liganden beider Targets trainiert. Die DrugBank, eine Datenbank zugelassener Wirkstoffe, dient hierbei als Hintergrundverteilung und stellt den Raum wirkstoffartiger chemischer Strukturen dar. Durch einen automatischen Vergleich der trainierten SOMs können mögliche gemeinsame Substrukturen identifiziert werden. Die Anwendung dieser Methode auf bekannte Inhibitoren der sEH und der 5-LO identifizierte neun Fragmente, die auf einem der beiden Targets, sowie fünf Fragmente welche auf beiden Targets im niedrigen mikromolaren Bereich inhibierend wirken. Eine Substruktursuche nach einem dieser Fragmente in einer internen Datenbank lieferte eine Verbindung, welche beide Targets im nanomolaren Bereich inhibiert und eine vielversprechender Basis als Leitstruktur für die Entwicklung dualer 5-LO/sEH-Inhibitoren darstellt.
Zusammenfassend wurden in dieser Arbeit mehrere Ansätze vorgestellt wie Pharmakophore in der Wirkstoffsuche eingesetzt werden können. Im Rahmen mehrerer Virtual Screenings konnten eine Reihe neuer Inhibitoren gefunden werden, einige mit nicht zuvor beschriebenen Strukturmerkmalen für das jeweilige Target. Es wurde außerdem eine neue Methode zur automatischen Generierung von Pharmakophor-Modellen entwickelt, welche sowohl retrospektiv als auch prospektiv validiert wurde.
We compute the probability distribution P(N) of the net-baryon number at finite temperature and quark-chemical potential, μ, at a physical value of the pion mass in the quark-meson model within the functional renormalization group scheme. For μ/T < 1, the model exhibits the chiral crossover transition which belongs to the universality class of the O(4) spin system in three dimensions. We explore the influence of the chiral crossover transition on the properties of the net baryon number probability distribution, P(N). By considering ratios of P(N) to the Skellam function, with the same mean and variance, we unravel the characteristic features of the distribution that are related to O(4) criticality at the chiral crossover transition. We explore the corresponding ratios for data obtained at RHIC by the STAR Collaboration and discuss their implications. We also examine O(4) criticality in the context of binomial and negative-binomial distributions for the net proton number.
Protein folding in cells is regulated by networks of chaperones, including the heat shock protein 70 (Hsp70) system, which consists of the Hsp40 cochaperone and a nucleotide exchange factor. Hsp40 mediates complex formation between Hsp70 and client proteins prior to interaction with Hsp90. We used mass spectrometry (MS) to monitor assemblies formed between eukaryotic Hsp90/Hsp70/Hsp40, Hop, p23, and a client protein, a fragment of the glucocorticoid receptor (GR). We found that Hsp40 promotes interactions between the client and Hsp70, and facilitates dimerization of monomeric Hsp70. This dimerization is antiparallel, stabilized by post-translational modifications (PTMs), and maintained in the stable heterohexameric client-loading complex Hsp902Hsp702HopGR identified here. Addition of p23 to this client-loading complex induces transfer of GR onto Hsp90 and leads to expulsion of Hop and Hsp70. Based on these results, we propose that Hsp70 antiparallel dimerization, stabilized by PTMs, positions the client for transfer from Hsp70 to Hsp90.
BACKGROUND: Vermeulen et al. 2014 published a meta-regression analysis of three relevant epidemiological US studies (Steenland et al. 1998, Garshick et al. 2012, Silverman et al. 2012) that estimated the association between occupational diesel engine exhaust (DEE) exposure and lung cancer mortality. The DEE exposure was measured as cumulative exposure to estimated respirable elemental carbon in μg/m(3)-years. Vermeulen et al. 2014 found a statistically significant dose-response association and described elevated lung cancer risks even at very low exposures.
METHODS: We performed an extended re-analysis using different modelling approaches (fixed and random effects regression analyses, Greenland/Longnecker method) and explored the impact of varying input data (modified coefficients of Garshick et al. 2012, results from Crump et al. 2015 replacing Silverman et al. 2012, modified analysis of Moehner et al. 2013).
RESULTS: We reproduced the individual and main meta-analytical results of Vermeulen et al. 2014. However, our analysis demonstrated a heterogeneity of the baseline relative risk levels between the three studies. This heterogeneity was reduced after the coefficients of Garshick et al. 2012 were modified while the dose coefficient dropped by an order of magnitude for this study and was far from being significant (P = 0.6). A (non-significant) threshold estimate for the cumulative DEE exposure was found at 150 μg/m(3)-years when extending the meta-analyses of the three studies by hockey-stick regression modelling (including the modified coefficients for Garshick et al. 2012). The data used by Vermeulen and colleagues led to the highest relative risk estimate across all sensitivity analyses performed. The lowest relative risk estimate was found after exclusion of the explorative study by Steenland et al. 1998 in a meta-regression analysis of Garshick et al. 2012 (modified), Silverman et al. 2012 (modified according to Crump et al. 2015) and Möhner et al. 2013. The meta-coefficient was estimated to be about 10-20 % of the main effect estimate in Vermeulen et al. 2014 in this analysis.
CONCLUSIONS: The findings of Vermeulen et al. 2014 should not be used without reservations in any risk assessments. This is particularly true for the low end of the exposure scale.
The RAF family of kinases constitutes the members A, B and CRAF. They mediate RAS signaling by linking it to the MEK/ERK transduction module, which regulates cellular processes such as cell proliferation, migration, survival and cell death. As the RAS/RAF/MEK/ERK (MAPK) pathway is found to be activated in human cancers, the RAF kinases have been exploited as valuable therapeutic targets and RAF inhibitors show promising results in the clinic, esp. with tumors harboring an activating BRAFV600E mutation. However, RAF inhibitors paradoxically accelerate metastasis in RAS mutant and BRAF wildtype tumors. They also become ineffective over time in BRAFV600E tumors because of reactivation of downstream mitogen-activated protein kinase (MAPK) signaling by promoting RAF dimerization. Aims of the present work were 1) to investigate the role of ARAF kinase in the paradoxical activation of the enzymatic cascade by RAF inhibitors downstream of mutated RAS and 2) to study the consequences of the loss of ARAF function on signal transduction in vitro and in vivo (nude mice). We have engineered several cell lines that would allow the study of basal and RAF inhibitor induced effects on MAPK activation, tumor cell migration and invasion.
In summary, we were able to show that the RAF isoform ARAF has an obligatory role in promoting MAPK activity and tumor cell invasion in a cell type dependent manner. In these cell types, ARAF depletion prevented the activation of MAPK kinase 1 (MEK1) and extracellular signal-regulated kinase 1 and 2 (ERK1/2) and led to a significant decrease of protrusions growing out of tumor cell spheroids in a three-dimensional (3D) culture that were otherwise induced by BRAFV600E-specific or BRAF/CRAF inhibitors (GDC-0879 and sorafenib, respectively). RAF inhibitors stimulated homodimerization of ARAF and heteromerization of BRAF with CRAF and the scaffolding protein KSR1. However, induced oligomerization was not sufficient to activate MAPK signaling if ARAF was depleted. By employing full length recombinant kinases, we were able to show for the first time that the three RAF isoforms competed for the binding to MEK1. In cell culture models, the overexpression of dimer-deficient ARAF mutants impaired the interaction between ARAF and endogenous MEK1 and thus prevented the subsequent phosphorylation of MEK1 and ERK1/2. Our findings reveal a new role for ARAF in directly activating the MAPK cascade through homodimerization and thereby promoting tumor cell invasion, suggesting the conserved RAF-dimer interface as a target for RAS- and RAF mediated cancer therapy.
Collectively, we provide evidence for the dual role ARAF plays in controlling MAPK signaling and cancer as loss of ARAF promoted strong lung metastasis formation in nude mice. Preliminary data describing the underlying mechanisms behind ARAF-regulated metastases have been presented and discussed.
Mechanisms regulating protein degradation ensure the correct and timely expression of transcription factors such as hypoxia inducible factor (HIF). Under normal O2 tension, HIFα subunits are targeted for proteasomal degradation, mainly through vHL-dependent ubiquitylation. Deubiquitylases are responsible for reversing this process. Although the mechanism and regulation of HIFα by ubiquitin-dependent proteasomal degradation has been the object of many studies, little is known about the role of deubiquitylases. Here, we show that expression of HIF2α (encoded by EPAS1) is regulated by the deubiquitylase Cezanne (also known as OTUD7B) in an E2F1-dependent manner. Knockdown of Cezanne downregulates HIF2α mRNA, protein and activity independently of hypoxia and proteasomal degradation. Mechanistically, expression of the HIF2α gene is controlled directly by E2F1, and Cezanne regulates the stability of E2F1. Exogenous E2F1 can rescue HIF2α transcript and protein expression when Cezanne is depleted. Taken together, these data reveal a novel mechanism for the regulation of the expression of HIF2α, demonstrating that the HIF2α promoter is regulated by E2F1 directly and that Cezanne regulates HIF2α expression through control of E2F1 levels. Our results thus suggest that HIF2α is controlled transcriptionally in a cell-cycle-dependent manner and in response to oncogenic signalling.
In search for the elusive schizophrenia pathway, candidate genes for the disorder from a discovery sample were localized within the energy-delivering and ischemia protection pathway. To test the adult vascular-ischemic (AVIH) and the competing neurodevelopmental hypothesis (NDH), functional genomic analyses of practically all available schizophrenia-associated genes from candidate gene, genome-wide association and postmortem expression studies were performed. Our results indicate a significant overrepresentation of genes involved in vascular function (P<0.001), vasoregulation (that is, perivascular (P<0.001) and shear stress (P<0.01), cerebral ischemia (P<0.001), neurodevelopment (P<0.001) and postischemic repair (P<0.001) among schizophrenia-associated genes from genetic association studies. These findings support both the NDH and the AVIH. The genes from postmortem studies showed an upregulation of vascular-ischemic genes (P=0.020) combined with downregulated synaptic (P=0.005) genes, and ND/repair (P=0.003) genes. Evidence for the AVIH and the NDH is critically discussed. We conclude that schizophrenia is probably a mild adult vascular-ischemic and postischemic repair disorder. Adult postischemic repair involves ND genes for adult neurogenesis, synaptic plasticity, glutamate and increased long-term potentiation of excitatory neurotransmission (i-LTP). Schizophrenia might be caused by the cerebral analog of microvascular angina.
The muscarinic M2 receptor (M2R) acts as a negative feedback regulator in central cholinergic systems. Activation of the M2 receptor limits acetylcholine (ACh) release, especially when ACh levels are increased because acetylcholinesterase (AChE) activity is acutely inhibited. Chronically high ACh levels in the extracellular space, however, were reported to down-regulate M2R to various degrees. In the present study, we used the PRiMA knockout mouse which develops severely reduced AChE activity postnatally to investigate ACh release, and we used microdialysis to investigate whether the function of M2R to reduce ACh release in vivo was impaired in adult PRiMA knockout mice. We first show that striatal and hippocampal ACh levels, while strongly increased, still respond to AChE inhibitors. Infusion or injection of oxotremorine, a muscarinic M2 agonist, reduced ACh levels in wild-type mice but did not significantly affect ACh levels in PRiMA knockout mice or in wild-type mice in which ACh levels were artificially increased by infusion of neostigmine. Scopolamine, a muscarinic antagonist, increased ACh levels in wild-type mice receiving neostigmine, but not in wild-type mice or in PRiMA knockout mice. These results demonstrate that M2R are dysfunctional and do not affect ACh levels in PRiMA knockout mice, likely because of down-regulation and/or loss of receptor-effector coupling. Remarkably, this loss of function does not affect cognitive functions in PRiMA knockout mice. Our results are discussed in the context of AChE inhibitor therapy as used in dementia.
Pharmacology: the pharmacodynamics of nutrients and nutrient interactions in biological functions
(2015)
Epidemiological studies and randomized controlled trials (RCTs) have shown that nutrition and nutritional habits may play a critical role in the optimal functioning of biological systems from conception to old age. Epidemiological studies, due to their methodology, can only provide correlations between consumption of nutrient(s) and biological outcomes, whereas RCTs normally study just one dose of a certain nutrient. Both study types are therefore ill-suited to study the mechanisms by which nutrients exert their benefits. Moreover, the nutrients’ functions may depend on each other. For example, B-vitamins’ functions are known to be interdependent. While the exact mechanisms are unclear, the course and severity of conditions such as obesity, cellular aging, cancer, and neurological disorders can be affected by nutritional approaches. Thus, food and nutrition play an intimate and inextricable role in human health. Despite growing interest in adequate nutrition, the effects of nutrient interaction, the possible varying effects on different organs, and the dependency of such effects on age or health status are complicated topics that deserve careful examination. ...
This article discusses obstacles to overcoming dangerous climate change. It employs an account of dangerous climate change that takes climate change and climate change policy as dangerous if it imposes avoidable costs of poverty prolongation. It then examines plausible accounts of the collective action problems that seem to explain the lack of ambition to mitigate. After criticizing the merits of two proposals to overcome these problems, it discusses the pledge and review process. It argues that pledge and review possesses the virtues of encouraging broad participation and of providing a procedural safeguard for the right of sustainable development. However, given the perceptions of the marginal short term costs of mitigation, pledge and review is unlikely, at least initially, to issue in an agreement to make deep reductions in greenhouse gas emissions. Because there is no rival approach that seems likely to better instantiate the two virtues, pledge and review may be the best available policy for mitigation. Moreover, recent economic research suggests that the co-benefits of mitigation may be greater than previously assumed and that the costs of renewable energy may be less than previously calculated. This would radically undermine claims that the short term mitigation costs necessarily render mitigation irrational and produce collective action problems. Given the circumstances, pledge and review might be our best hope to avoid dangerous climate change.
The upcoming CBM Experiment at FAIR aims at exploring the region of highest net baryonic densities reproducible in energetic heavy ion collisions. Due to the very high beam intensities expected at FAIR, unprecedented data regarding rare observables such as charm quarks and hyperons will be accessible. Open charm mesons are particularly interesting, since they support the reconstruction of the total charm cross-section in order to search for exotic phenomena, e.g. a phase transition towards the quark-gluon plasma which is predicted by several theoretical models. Open charm studies will be performed via secondary vertex reconstruction with a suitable Micro-Vertex Detector (MVD). The CBM-MVD is currently in the development and prototyping phase with primary design goals concentrating on spatial resolution, radiation hardness, material budget, and readout performance. CMOS Monolithic Active Pixel Sensors (MAPS) provide an excellent spatial resolution for the MVD in the order of few um in combination with a low material budget (50 um thickness) and high radiation hardness. The active volume of the devices is formed from the epitaxial layer of standard CMOS wafers. This allows for integration of pixels together with analogue and digital data processing circuits on one single chip. This option was explored with the MIMOSA-26 prototype, which integrates functionalities like pedestal correction, correlated double sampling, discrimination and data sparsification based on zero suppression combined with a small and dense pixel matrix. The pixel array composed of 576 lines of 1152 pixels is read out in a column-parallel rolling shutter mode. One discriminator per column and the digital data processing circuits are located on the same chip in a 3 mm wide area beneath the pixel matrix allowing for binary hit encoding. This area also contains the circuits for pedestal correction and the configuration memory, which is programmed via JTAG. The preprocessed digital data is read out via two 80 Mbit/s LVDS links per sensor, which stream their data continuously based on a low-level protocol.
Within the scope of this thesis, a readout concept of the CBM-MVD is proposed and studied based on the current MIMOSA sensor generation. The backbone of the system is formed by the Readout Controller boards (ROCs) featuring FPGA microchips and optical links. Several ROC prototypes are considered using the synergy with the HADES Experiment. Finally, the TRB3 board is selected as a possible candidate for the initial FAIR experiments. Furthermore, a highly scalable, hardware independent FPGA firmware is implemented in order to steer and read out multiple MIMOSA-26 sensors. The reconfigurable firmware is also designed with the support for future MIMOSA sensor generations. The free-streaming sensor data is deserialized and error-checked, prior to its transmission over a suitable network interface. In order to demonstrate the validity of the concept, a readout network similar to the HADES Data Acquisition (DAQ) system is developed. The ROC is tested on the HADES TRB2 boards and data is acquired using suitable MAPS add-on boards and the TrbNet protocol.
In the context of the CBM-MVD prototype project, a readout network with 12 MIMOSA-26 sensors has been prepared for an in-beam test at the CERN SPS facility. A comprehensive control system is designed comprising customized software tools. The subsequent in-beam test is used to validate the design choices. As a result, the system could be operated synchronously and dead-time free for several days. The readout network behavior in a realistic operating environment has been carefully studied with the outcome the the TrbNet based approach handles the MVD prototype setup without any difficulties. A procedure to keep the sensors synchronous even in case of a data overflow has been pioneered as well. After the beam test, improvements and conceptual changes to the readout systems are being addressed which allow an integration into the global CBM DAQ system.
Background: Recently, we have shown that the ATP-binding cassette (ABC) transporter ABCB1 interferes with the anti-cancer activity of the pan-aurora kinase inhibitor tozasertib (VX680, MK-0457) but not of the aurora kinase A and B inhibitor alisertib (MLN8237). Preliminary data had suggested tozasertib also to be a substrate of the ABC transporter ABCG2, another ABC transporter potentially involved in cancer cell drug resistance. Here, we studied the effect of ABCG2 on the activity of tozasertib and alisertib.
Results: The tozasertib concentration that reduces cell viability by 50 % (IC50) was dramatically increased in ABCG2-transduced UKF-NB-3ABCG2 cells (48.8-fold) compared to UKF-NB-3 cells and vector-transduced control cells. The ABCG2 inhibitor WK-X-34 reduced tozasertib IC50 to the level of non-ABCG2-expressing UKF-NB-3 cells. Furthermore, ABCG2 depletion from UKF-NB-3ABCG2 cells using another lentiviral vector expressing an shRNA against the bicistronic mRNA of ABCG2 and eGFP largely re-sensitised these cells to tozasertib. In contrast, alisertib activity was not affected by ABCG2 expression.
Conclusions: Tozasertib but not alisertib activity is affected by ABCG2 expression. This should be considered within the design and analysis of experiments and clinical trials investigating these compounds.
The PKCβ inhibitor enzastaurin was tested in parental neuroblastoma and rhabdomyosarcoma cell lines, their vincristine-resistant sub-lines, primary neuroblastoma cells, ABCB1-transduced, ABCG2-transduced, and p53-depleted cells. Enzastaurin IC50s ranged from 3.3 to 9.5 μM in cell lines and primary cells independently of the ABCB1, ABCG2, or p53 status. Enzastaurin 0.3125 μM interfered with ABCB1-mediated drug transport. PKCα and PKCβ may phosphorylate and activate ABCB1 under the control of p53. However, enzastaurin exerted similar effects on ABCB1 in the presence or absence of functional p53. Also, enzastaurin inhibited PKC signalling only in concentrations ≥ 1.25 μM. The investigated cell lines did not express PKCβ. PKCα depletion reduced PKC signalling but did not affect ABCB1 activity. Intracellular levels of the fluorescent ABCB1 substrate rhodamine 123 rapidly decreased after wash-out of extracellular enzastaurin, and enzastaurin induced ABCB1 ATPase activity resembling the ABCB1 substrate verapamil. Computational docking experiments detected a direct interaction of enzastaurin and ABCB1. These data suggest that enzastaurin directly interferes with ABCB1 function. Enzastaurin further inhibited ABCG2-mediated drug transport but by a different mechanism since it reduced ABCG2 ATPase activity. These findings are important for the further development of therapies combining enzastaurin with ABC transporter substrates.
Im Juni spricht der Leipziger Schriftsteller Clemens Meyer im Rahmen der Frankfurter Poetikvorlesungen über den „Untergang der Äkschn GmbH“. Meyers ungewöhnliche Biographie und seine Romane über Leipziger Jugendgangs, Prostituierte und Zuhälter versprechen interessante Vorträge. Wir haben ihm vorab einige Fragen gestellt – seine mitunter forschen Antworten deuten jedenfalls an, dass der Autor sein Publikum bestimmt nicht langweilen wird.
Im Schulunterricht der deutschen Gymnasien hat die Vermittlung poetologischen Wissens im 19. Jahrhundert einen besonderen Platz eingenommen. Dabei wurde das Gebiet der Poetik jedoch sehr unterschiedlich dargestellt. Zum einen war die Poetik, die Lehre der Dichtkunst, seit dem 18. und während des gesamten 19. Jahrhunderts fortlaufend Veränderungen und Repositionierungen unterworfen. Zum anderen formte und entwickelte sich der moderne Deutschunterricht in dieser Zeit, stark beeinflusst durch die zeitgeschichtlichen Tendenzen der Verwissenschaftlichung, der Fächerdifferenzierung und der Nationalideologien. Als Konstante lässt sich jedoch über das gesamte Jahrhundert hinweg eine hohe Wertschätzung der Poetik als Unterrichtsfach erkennen. Daher wurden von Schulbuchverlagen von Beginn des 19. und bis in die 20er Jahre des folgenden Jahrhunderts hinein didaktische Poetiken veröffentlicht, die eine sehr lange und weite schulische Verwendung fanden.
In der hier vorgelegten Arbeit werden anhand einer Auswahl dieser Schulpoetiken die Grundargumente des Diskurses über Poetik herausgearbeitet und untersucht, wie sich diese im Laufe des Jahrhunderts veränderten. Dadurch wird eine Grundlage dafür geschaffen, das als gültig wahrgenommene Wissen über Form und Wesen der Literatur zu rekonstruieren, das sowohl die Leser aber auch die Schriftsteller beeinflusst hat, die aus den Schülergenerationen zwischen 1830 und 1920 stammen.
Nach der Landtagswahl in Bremen 2007 haben sich, nach langjähriger SPD/CDU-Partnerschaft (1995-2007), zwei Parteien zu einer Koalition entschlossen, die in ihren Wahlprogrammen eine „Schule für alle“ (Grüne) bzw. eine „Gemeinsame Schule“ (SPD) von 5 bis 10 angekündigt haben. Die Befürworter einer solchen Schule erwarteten, dass den Ankündigungen im Wahlkampf nun auch Taten folgen. So forderte die GEW von SPD und Grünen die als ersten Schritt versprochenen Maßnahmen: Alle Schulen werden verpflichtet, „die aufgenommenen Schülerinnen und Schüler in ihrer Schule zu einem Abschluss zu führen“ (SPD) und alle Abschlüsse der Sekundarstufe I können „an jeder Schule erworben werden“ (Grüne), womit alle Bildungsgänge, das Gymnasium eingeschlossen, bei der Entwicklung eines integrativen Schulsystems einbezogen waren...
In der familienbiographischen Studie „Bürgerliche Lebenswelten im Spiegel eines familiären Briefwechsels“ wird eine bürgerliche, nicht-prominente Familie aus Hamburg über drei Generationen hinweg in der Zeit von 1840 bis 1930 untersucht. Als Quellen wurden knapp 3000 Privatbriefe sowie mehrere Familienchroniken ausgewertet.
Thematisch gehört die Arbeit zum Kontext der deutschsprachigen Bürgertumsforschung und hat eine Schnittmenge mit mehreren thematischen Unterbereichen: Sie legt einen starken Fokus auf geschlechtergeschichtliche Themen und Problemstellungen und weist interdisziplinär Schnittmengen mit der Soziologie auf. Gerade bei der Beschreibung von biographisch hochemotionalen Momenten nähert sie sich bewusst der bislang wenig beachteten ,Gefühlskultur’ bürgerlicher Menschen und ihrer je nach Persönlichkeit sehr individuellen Ausprägung an.
Desde Dialéctica de la Ilustración hasta Dialéctica negativa, el materialismo filosófico llevado adelante por T. W. Adorno ha ubicado en un lugar central de sus reflexiones la problemática de lo corporal, poniéndolo en discusión directa tanto con el psicoanálisis y su teoría de las pulsiones, así como con las diferentes versiones del idealismo. La reflexión acerca de este ámbito, permitirá exponer tanto el carácter represivo de la sociedad; también, la posibilidad de una ética verdaderamente democrática.
The presented work inside this thesis aims to raise the degree of automation in analog circuit design. Therefore, a framework was developed to provide the necessary mechanisms in order to carry out a fully automated analog circuit synthesis, i.e., the construction of an analog circuit fulfilling all previously defined (electrical) specifications. Nowadays, analog circuit design in general is a very time consuming process compared to a digital design flow. Due to its discrete nature, the digital design process is highly automated and thus very efficient compared to analog circuit design. In modern Very-Large-Scale integration (VLSI) circuits the analog parts are mostly just a small portion of the overall chip area. Although this small portion is known to consume a major part of the needed workforce. Paired with product cycles which constantly get shorter, the time needed to develop the analog parts of an integrated circuit (IC) becomes a determinant factor. Apart from this, the ongoing progress in semiconductor processing technologies promises more speed with less power consumption on smaller areas, forcing the IC developers to keep track with the technology nodes in order to maintain competitiveness. Analog circuitry exhibits the inherent property of being hard to reuse, as porting from one technology node to another imposes critical changes for operating conditions (e.g., supply voltage) - mostly leading to a full redesign for most of the analog modules. This productivity gap between digital and analog design resembles the primary motivation for this thesis. Due to the availability of commercial sizing tools, this work deliberately focuses on the construction of circuit topologies in distinction to parameter synthesis, which can be obtained with a dedicated sizing tool. The focus on circuit construction allows the development of a framework which allows a full design space exploration. This thesis describes the needed concepts and methods to realize a deterministic, explorative analog synthesis framework. Despite this, a reference implementation is presented, which demonstrates the applicability in current analog design flows.
This paper provides a theoretical assessment of gestures in the context of authoring image-related hypertexts by example of the museum information system WikiNect. To this end, a first implementation of gestural writing based on image schemata is provided (Lakoff in Women, fire, and dangerous things: what categories reveal about the mind. University of Chicago Press, Chicago, 1987). Gestural writing is defined as a sort of coding in which propositions are only expressed by means of gestures. In this respect, it is shown that image schemata allow for bridging between natural language predicates and gestural manifestations. Further, it is demonstrated that gestural writing primarily focuses on the perceptual level of image descriptions (Hollink et al. in Int J Hum Comput Stud 61(5):601–626, 2004). By exploring the metaphorical potential of image schemata, it is finally illustrated how to extend the expressiveness of gestural writing in order to reach the conceptual level of image descriptions. In this context, the paper paves the way for implementing museum information systems like WikiNect as systems of kinetic hypertext authoring based on full-fledged gestural writing.
A wide variety of enzymatic pathways that produce specialized metabolites in bacteria, fungi and plants are known to be encoded in biosynthetic gene clusters. Information about these clusters, pathways and metabolites is currently dispersed throughout the literature, making it difficult to exploit. To facilitate consistent and systematic deposition and retrieval of data on biosynthetic gene clusters, we propose the Minimum Information about a Biosynthetic Gene cluster (MIBiG) data standard.
The assumed space : pre-reflective spatiality and doctrinal configurations in juridical experience
(2015)
The purpose of this contribution is to analyse, by means of the legal-historical perspective, the relationship between the pre-reflections of space and the configurations of legal concepts and categories. Three examples of the interplay between doctrinal configurations and the spatial dimension within the context of three different historical periods will be illustrated: given space in the Middle Ages, possible space in the Modern Age and decided space in the Contemporary Age. From this basis, the essay considers the heuristic importance of such an analytical approach – mindful of the profiles of presupposition, such as the space assumption, underlying the conceptualisation of ideas – for a history attentive to the constraints of the theoretical sustainability of legal concepts.
Leaky integrate-and-fire (LIF) network models are commonly used to study how the spiking dynamics of neural networks changes with stimuli, tasks or dynamic network states. However, neurophysiological studies in vivo often rather measure the mass activity of neuronal microcircuits with the local field potential (LFP). Given that LFPs are generated by spatially separated currents across the neuronal membrane, they cannot be computed directly from quantities defined in models of point-like LIF neurons. Here, we explore the best approximation for predicting the LFP based on standard output from point-neuron LIF networks. To search for this best “LFP proxy”, we compared LFP predictions from candidate proxies based on LIF network output (e.g, firing rates, membrane potentials, synaptic currents) with “ground-truth” LFP obtained when the LIF network synaptic input currents were injected into an analogous three-dimensional (3D) network model of multi-compartmental neurons with realistic morphology, spatial distributions of somata and synapses. We found that a specific fixed linear combination of the LIF synaptic currents provided an accurate LFP proxy, accounting for most of the variance of the LFP time course observed in the 3D network for all recording locations. This proxy performed well over a broad set of conditions, including substantial variations of the neuronal morphologies. Our results provide a simple formula for estimating the time course of the LFP from LIF network simulations in cases where a single pyramidal population dominates the LFP generation, and thereby facilitate quantitative comparison between computational models and experimental LFP recordings in vivo.
Para responder a la pregunta: ¿Qué es la literatura?, Sartre propone el concepto de unidad como su característica exclusiva que la relaciona con la sociedad por la vía del compromiso. Se analiza tal exclusividad, así como las objeciones de Adorno a la noción de compromiso, para encontrar, en medio de sus grandes diferencias, algunas afinidades que permitan establecer las relaciones entre la literatura y la sociedad.
This chapter outlines the conditions under which accounting-based smoothing can be beneficial for policyholders who hold with-profit or participating payout life annuities (PLAs). We use a realistically-calibrated model of PLAs to explore how alternative accounting techniques influence policyholder welfare as well as insurer profitability and stability. We find that accounting smoothing of participating life annuities is favorable to consumers and insurers, as it mitigates the impact of short-term volatility and enhances the utility of these long-term annuity contracts.
This paper investigates whether exchanging the Social Security delayed retirement credit, currently paid as an increase in lifetime annuity benefits, for a lump sum would induce later claiming and additional work. We show that people would voluntarily claim about half a year later if the lump sum were paid for claiming any time after the Early Retirement Age, and about two-thirds of a year later if the lump sum were paid only for those claiming after their Full Retirement Age. Overall, people will work one-third to one-half of the additional months, compared to the status quo. Those who would currently claim at the youngest ages are likely to be most responsive to the offer of a lump sum benefit.
The paper discusses an additional reform proposal for enhancing Social Security solvency which reframes the existing debate in a different light. In our research, we focus on incentives to prolong working years and to delay benefits claiming as a way of sustaining Social Security. Specifically, we analyze how the offer of a budget-neutral, actuarially fair lump sum payment - instead of the current delayed retirement credit – would encourage people to delay claiming their OASI benefits and work longer. The results of our research will be useful for policymakers, namely in (1) measuring who would delay claiming benefits if offered a lump sum instead of higher annuity payments, (2) examining how long they would wait, and (3) how much longer, if at all, they would continue working in the interim.
Introduction: The effects of manipulated dental occlusion on body posture has been investigated quite often and discussed controversially in the literature. Far less attention has been paid to the influence of dental occlusion position on human movement. If human movement was analysed, it was mostly while walking and not while running. This study was therefore designed to identify the effect of lower jaw positions on running behaviour according to different dental occlusion positions.
Methods: Twenty healthy young recreational runners (mean age = 33.9±5.8 years) participated in this study. Kinematic data were collected using an eight-camera Vicon motion capture system (VICON Motion Systems, Oxford, UK). Subjects were consecutively prepared with four different dental occlusion conditions in random order and performed five running trials per test condition on a level walkway with their preferred running shoes. Vector based pattern recognition methods, in particular cluster analysis and support vector machines (SVM) were used for movement pattern identification.
Results: Subjects exhibited unique movement patterns leading to 18 clusters for the 20 subjects. No overall classification of the splint condition could be observed. Within individual subjects different running patterns could be identified for the four splint conditions. The splint conditions lead to a more symmetrical running pattern than the control condition.
Discussion: The influence of an occlusal splint on running pattern can be confirmed in this study. Wearing a splint increases the symmetry of the running pattern. A more symmetrical running pattern might help to reduce the risk of injuries or help in performance. The change of the movement pattern between the neutral condition and any of the three splint conditions was significant within subjects but not across subjects. Therefore the dental splint has a measureable influence on the running pattern of subjects, however subjects individuality has to be considered when choosing the optimal splint condition for a specific subject.
Diabetes-assoziierte Fußulzerationen (diabetic foot ulcerations, DFU) repräsentieren eine schwerwiegende klinische Komplikation der Wundheilung. Bislang sind pharmakologische Behandlungsansätze diabetischer Wundheilungsstörung unzureichend und limitiert. Der Erkenntnismangel der zugrundeliegenden zellulären und molekularen Mechanismen gestörter Wundheilung ergänzt die unzufrieden stellende klinische Situation. In den vergangenen Jahren sind vermehrt zelluläre Wundverbände in den klinischen Fokus gerückt. Sie ermöglichen eine individuelle, dynamische Wundbehandlung und haben in den ersten klinischen Studien vielversprechende Ergebnisse gezeigt.
In der vorliegenden Arbeit ist ein zellulärer Wundverband der Firma Boehringer Ingelheim genutzt worden, um die Wundheilung in diabetischen db/db-Tieren zu analysieren. Der Wundverband (BAWD; biological active wound dressing) besteht aus humanen Keratinozyten, die auf einer Hyaluronsäure-haltigen Matrix kultiviert werden.
Nach topischer Anwendung der lebenden Wundauflage war eine Interaktion humaner Keratinozyten mit murinem Wundgewebe zu beobachten. Die gestörte diabetische Wundheilung in der db/db-Maus war nach BAWD-Behandlung in einem um 30 % verbesserten Wundverschluss und dem Aufbau qualitativ neuen Gewebes deutlich verbessert.
Aufgrund der unverändert hohen Expression von Zyto- und Chemokinen in der frühen und späten Heilungsphase wurde eine Dämpfung der Immunantwort ausgeschlossen. Vielmehr war eine BAWD-vermittelte differenzielle Immunzellverteilung festzuhalten. Zudem zeigten Whole-Genom-Sequenzanalysen eine BAWD-induzierte Expression von Genen auf, die regenerative M2-ähnliche M[Phi] charakterisieren.
Außerdem scheint die BAWD-Anwendung nach Auswertung immunhistochemischer Daten und über die signifikant erhöhte CD29-, CD44- und Sca1-mRNA-Expression die Rekrutierung heilungsfördernder MSCs zu begünstigen, denen ein potentiell anti-entzündlicher Charakter zugesprochen wird.
In dieser Arbeit konnte zudem ein neuer Regelkreis kutaner Wundheilung beschrieben werden, der auf Basis der Expression muskelspezifischer Faktoren und der transienten Ausbildung kontraktiler Elemente in der Wunde normal heilender Tiere beruht, die bislang nicht beschrieben wurden. Interessanterweise induzierte eine BAWD-Anwendung die Expression muskelspezifischer Gene und Proteine in der Wundheilung diabetischer Tiere. Möglicherweise stellt die Ausbildung kontraktiler Elemente neben der Differenzierung von Fibroblasten zu Myofibroblasten eine ergänzende Komponente für einen beschleunigten Wundverschluss dar. Diese Befunde eröffnen neue Möglichkeiten zu Verständnis und Therapie diabetischer gestörter Wundheilung im humanen Organismus.
Biodiversity is unevenly distributed on Earth. Highly diverse biotas are particularly expected in mountain systems, because altitudinal zonation provides a number of habitat alternatives, which could lead to lower extinction rates during climatic changes. Nevertheless, the impact of environmental changes on plant diversification (especially for sub-alpine taxa) in the course of mountain orogenesis remains poorly understood. This is also true for the highest and largest plateau on Earth, the Qinghai-Tibetan Plateau (QTP) and its surrounding areas.In this doctoral thesis, I investigated the impact of environmental changes on plant diversification and the floristic exchange between the QTP region and biodiversity hotspots of Southeast Asia as well as other parts of the world by using the sub-alpine genera Agapetes and Vaccinium (Vaccinieae, Ericaceae) as well as Tripterospermum (Gentianinae, Gentianaceae) as model systems. Furthermore, I examined the role of niche evolution and conservatism in a changing environment over time, and detected possible beneficial morphological traits of plants in the surroundings of the QTP by investigating subtropical Gentianinae (Crawfurdia, Kuepferia, Metagentiana, Sinogentiana, and Tripterospermum; Gentianaceae).
Bei der hier anzuzeigenden Monographie handelt es sich um die Habilitationsschrift von St. F. P(fahl), mit der er 2011 im Fach Alte Geschichte unter besonderer Berücksichtigung der historischen Hilfswissenschaften an der Heinrich-Heine Universität Düsseldorf habilitiert wurde. Die Dissertation und die weiteren Veröffentlichungen weisen den Autor als provinzialrömischen Archäologen aus...
Der im Folgenden anzuzeigende Band ist aus der Tagung „Oratory and Politics in the Roman Republic“ hervorgegangen, die im September 2010 in Oxford veranstaltet wurde. Die Herausgeberinnen stellen in der „Introduction“ (1-7) heraus, dass man politische Reden zwar bislang durchaus untersucht, die Wirkung derselben aber eher vernachlässigt habe. Diesem Aspekt ist der Band gewidmet (2). Ferner stünden diesmal nicht Ciceros Reden im Zentrum der folgenden Artikel. Statt dessen habe man sich bewusst auf die weniger gut belegten orationes anderer Politiker konzentriert. Ein wichtiges, aber kaum überraschendes Ergebnis wird bereits hier verkündet: Zwar habe der römische Redner mit seinem Vortrag politischen Einfluss ausüben wollen, doch sei der Effekt einer Rede nicht immer vorhersehbar gewesen (2). Ein weiteres Resultat erstaunt ebenso wenig: Die Rhetorik habe in der politischen Karriere der römischen Politiker zum Teil ganz unterschiedlichen Zielen gedient. Cicero erscheine dabei in mehrfacher Hinsicht als Ausnahme, „both in his near-exclusive dependence on oratory to fuel his public career, and in the choices he makes about how to use oratory. […] and he exploited to an exceptionally high degree the possibility of preserving his oratory in textual form“ (3). Mit anderen Worten, die Sonderstellung Ciceros als erfolgreicher Redner wird erneut betont. Kurze Zusammenfassungen der insgesamt 19 Beiträge schließen die Einführung ab (4-6). Letzteres macht eine kurze Besprechung sämtlicher Artikel obsolet. Statt dessen sollen im Folgenden einzelne Studien detaillierter besprochen werden...
Eine Monographie zur Geschichte der römischen Provinz Germania Superior existiert bislang nicht, wenngleich zahlreiche Artikel, Einzelstudien und auch Bücher sich mit einzelnen Aspekten oder der Provinz insgesamt beschäftigen. Insofern kann man dem Klappentext des hier besprochenen Buches von M. K(lee) durchaus zustimmen, dass es sich um eine „längst überfällige“ Studie handelt, wobei zugleich ein „neuer Blick“ auf die „Gründung und Entwicklung“ der Provinz versprochen wird...
Rezension zu: Alison E. Cooley, The Cambridge Manual of Latin Epigraphy (Cambridge u.a. 2012)
(2015)
Background: Due to the large amount of data produced by advanced microscopy, automated image analysis is crucial in modern biology. Most applications require reliable cell nuclei segmentation. However, in many biological specimens cell nuclei are densely packed and appear to touch one another in the images. Therefore, a major difficulty of three-dimensional cell nuclei segmentation is the decomposition of cell nuclei that apparently touch each other. Current methods are highly adapted to a certain biological specimen or a specific microscope. They do not ensure similarly accurate segmentation performance, i.e. their robustness for different datasets is not guaranteed. Hence, these methods require elaborate adjustments to each dataset.
Results: We present an advanced three-dimensional cell nuclei segmentation algorithm that is accurate and robust. Our approach combines local adaptive pre-processing with decomposition based on Lines-of-Sight (LoS) to separate apparently touching cell nuclei into approximately convex parts. We demonstrate the superior performance of our algorithm using data from different specimens recorded with different microscopes. The three-dimensional images were recorded with confocal and light sheet-based fluorescence microscopes. The specimens are an early mouse embryo and two different cellular spheroids. We compared the segmentation accuracy of our algorithm with ground truth data for the test images and results from state-of-the-art methods. The analysis shows that our method is accurate throughout all test datasets (mean F-measure: 91%) whereas the other methods each failed for at least one dataset (F-measure≤69%). Furthermore, nuclei volume measurements are improved for LoS decomposition. The state-of-the-art methods required laborious adjustments of parameter values to achieve these results. Our LoS algorithm did not require parameter value adjustments. The accurate performance was achieved with one fixed set of parameter values.
Conclusion: We developed a novel and fully automated three-dimensional cell nuclei segmentation method incorporating LoS decomposition. LoS are easily accessible features that ensure correct splitting of apparently touching cell nuclei independent of their shape, size or intensity. Our method showed superior performance compared to state-of-the-art methods, performing accurately for a variety of test images. Hence, our LoS approach can be readily applied to quantitative evaluation in drug testing, developmental and cell biology.
The standard view suggests that removing barriers to entry and improving judicial enforcement reduces informality and boosts investment and growth. However, a general equilibrium approach shows that this conclusion may hold to a lesser extent in countries with a constrained supply of funds because of, for example, a more concentrated banking sector or lower financial openness. When the formal sector grows larger in those countries, more entrepreneurs become creditworthy, but the higher pressure on the credit market limits further capital accumulation. We show empirical evidence consistent with these predictions.
After the mass-vaccination campaign during the influenza A (H1N1) 2009 pandemic, a significant increase in narcolepsy incidence was observed initially in Scandinavia, later in other European countries and recently also in Canada. Narcolepsy is a sleep disease caused by the loss of hypocretin-producing cells in the hypothalamus. Almost all narcolepsy patients carry the HLA-DQB1*0602 allele, giving a link to an autoimmune-mediated process.
Most of the observed narcolepsy cases were correlated to the vaccination with Pandemrix, the most frequently used vaccine in the EU, and a slight connection to Arepanrix was also detected, which was distributed in Canada. Both vaccines were adjuvanted with AS03, suggesting a possible link between AS03 and narcolepsy. No narcolepsy cases were detected with MF59-adjuvanted or non-adjuvanted influenza vaccines. Recent studies reported differences between Pandemrix and Arepanrix and suggested the vaccine rather than the adjuvant as a suspect for narcolepsy development following vaccination. In addition, in China an increase of narcolepsy cases was reported to occur in absence of vaccination. Possible factors and potential additive effects that may have triggered narcolepsy after the pandemic vaccination are being reviewed in this paper.
Adorno und die Kabbala
(2015)
Im neunten Band der Reihe geht Ansgar Martins kabbalistischen Spuren in der Philosophie Theodor W. Adornos (1903–1969) nach. Der Frankfurter Gesellschaftskritiker griff im Rahmen seines radikalen materialistischen Projekts gleichwohl auch auf "theologische" Deutungsfiguren zurück. Vermittelt durch den gemeinsamen Freund Walter Benjamin (1892–1940) stieß Adorno dabei auf das Werk des Kabbala-Forschers Gershom Scholem (1897–1982). Zwischen Frankfurt und Jerusalem entwickelte sich eine lebenslange Korrespondenz.
Für Adorno erscheint vor dem Hintergrund lückenloser kapitalistischer Vergesellschaftung jede religiöse Sinngebung in der Moderne als unmöglich. Der Tradition der jüdischen Mystik schreibt er hingegen eine innere Affinität zu dieser hoffnungslosen Logik des "Verfalls" zu. Sie scheint ihm zur unumgänglichen Säkularisierung religiöser Gehalte aufzufordern. Adornos kabbalistische Marginalien beziehen einen breiten Horizont jüdisch-messianischer Ideen ein. Er verleugnet dabei nie, dass es ihm um eine sehr diesseite Verwirklichung geoffenbarter Heilsversprechen zu tun ist: Transzendenz sei als erfüllte Immanenz, als verwirklichte Utopie zu denken. In diesem Anliegen sieht Adorno selbst jedoch gerade seine Übereinstimmung mit der Kabbala.
Adornos kabbalistische Motive, die auf Scholems Forschungen zurückgehen, werden hier ausführlich an seinen Schriften und Vorlesungen untersucht. In seinem Verständnis der philosophischen Tradition sowie im Modell der Metaphysischen Erfahrung suchte er etwa explizit Anschluss an Deutungen der Kabbala: Das unerreichbare Urbild der Philosophie sei die Interpretation der geoffenbarten Schrift. Wie säkularisierte heilige Texte wurden Werke von Beethoven, Goethe, Kafka oder Schönberg so zum Anlass für "mystische" Interpretationen. Deren detaillierte Untersuchung erlaubt, das viel beschworene jüdische Erbe von Adornos Philosophie zu konkretisieren und bedenkenswerte Einzelheiten von der Negativen Dialektik zur Ästhetik in den Blick zu nehmen.
Incidence rates of clinically significant tinnitus: 10-year trend from a cohort study in England
(2015)
Objective: To investigate the incidence of tinnitus that burdens the health service in England.
Design: This was an observational study of 4.7 million residents of England under 85 years of age who were at risk for developing clinically significant tinnitus (sigT). SigT was defined by a discharge from hospital with a primary diagnosis of tinnitus, or a primary care recording of tinnitus with subsequent related medical follow-up within 28 days. The database used was the Clinical Practice Research Datalink and individual records were linked to additional data from the Hospital Episode Statistics. The observational period was from January 1, 2002 to December 31, 2011. Age-, gender-, and calendar year-specific incidence rates for and cumulative incidences of sigT were estimated and a projection of new cases of sigT between 2012 and 2021 was performed.
Results: There were 14,303 incident cases of sigT identified among 26.5 million person-years of observation. The incidence rate was 5.4 new cases of sigT per 10,000 person-years (95% confidence interval: 5.3 to 5.5). The incidence rate did not depend on gender but increased with age, peaking at 11.4 per 10,000 in the age group 60 to 69 years. The annual incidence rate of sigT increased from 4.5 per 10,000 person-years in 2002 to 6.6 per 10,000 person-years in 2011. The 10-year cumulative incidence of sigT was 58.4 cases (95% confidence interval: 57.4 to 59.4) per 10,000 residents. Nearly 324,000 new cases of sigT are expected to occur in England between 2012 and 2021.
Conclusions: Tinnitus presents a burden to the health care system that has been rising in recent years. Population-based studies provide crucial underpinning evidence; highlighting the need for further research to address issues around effective diagnosis and clinical management of this heterogeneous condition.