TY - THES A1 - Büntemeyer, Tjark-Ole T1 - Wertigkeit der Leberresektion bei Metastasen des Nebennierenkarzinoms - Analyse anhand des Deutschen Nebennierenkarzinom-Registers T1 - Role of Liverresection in adrenocortical carcinoma liver metastases N2 - Patienten mit einem hepatisch metastasierten Nebennierenkarzinom und ohne Hinweise auf extrahepatische Tumormanifestationen profitieren von einer Operation im Hinblick auf das Gesamtüberleben. Dies gilt sowohl für synchron- als auch für metachron metastasierte Patienten. N2 - Liver resection in case of ACC liver metastases can achieve long term survival, but disease free survival is short despite metastasectomy. Time to recurrence is a predictive factor for the outcome. KW - Nebenniere KW - Leberresektion KW - Nebennierenkarzinom Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-155743 ER - TY - THES A1 - Leimbach, Andreas T1 - Genomics of pathogenic and commensal \(Escherichia\) \(coli\) T1 - Genomik pathogener und kommensaler \(Escherichia\) \(coli\) N2 - High-throughput sequencing (HTS) has revolutionized bacterial genomics. Its unparalleled sensitivity has opened the door to analyzing bacterial evolution and population genomics, dispersion of mobile genetic elements (MGEs), and within-host adaptation of pathogens, such as Escherichia coli. One of the defining characteristics of intestinal pathogenic E. coli (IPEC) pathotypes is a specific repertoire of virulence factors (VFs). Many of these IPEC VFs are used as typing markers in public health laboratories to monitor outbreaks and guide treatment options. Instead, extraintestinal pathogenic E. coli (ExPEC) isolates are genotypically diverse and harbor a varied set of VFs -- the majority of which also function as fitness factors (FFs) for gastrointestinal colonization. The aim of this thesis was the genomic characterization of pathogenic and commensal E. coli with respect to their virulence- and antibiotic resistance-associated gene content as well as phylogenetic background. In order to conduct the comparative analyses, I created a database of E. coli VFs, ecoli_VF_collection, with a focus on ExPEC virulence-associated proteins (Leimbach, 2016b). Furthermore, I wrote a suite of scripts and pipelines, bac-genomics-scripts, that are useful for bacterial genomics (Leimbach, 2016a). This compilation includes tools for assembly and annotation as well as comparative genomics analyses, like multi-locus sequence typing (MLST), assignment of Clusters of Orthologous Groups (COG) categories, searching for protein homologs, detection of genomic regions of difference (RODs), and calculating pan-genome-wide association statistics. Using these tools we were able to determine the prevalence of 18 autotransporters (ATs) in a large, phylogenetically heterogeneous strain panel and demonstrate that many AT proteins are not associated with E. coli pathotypes. According to multivariate analyses and statistics the distribution of AT variants is instead significantly dependent on phylogenetic lineages. As a consequence, ATs are not suitable to serve as pathotype markers (Zude et al., 2014). During the German Shiga toxin-producing E. coli (STEC) outbreak in 2011, the largest to date, we were one of the teams capable of analyzing the genomic features of two isolates. Based on MLST and detection of orthologous proteins to known E. coli reference genomes the close phylogenetic relationship and overall genome similarity to enteroaggregative E. coli (EAEC) 55989 was revealed. In particular, we identified VFs of both STEC and EAEC pathotypes, most importantly the prophage-encoded Shiga toxin (Stx) and the pAA-type plasmid harboring aggregative adherence fimbriae. As a result, we could show that the epidemic was caused by an unusual hybrid pathotype of the O104:H4 serotype. Moreover, we detected the basis of the antibiotic multi-resistant phenotype on an extended-spectrum beta-lactamase (ESBL) plasmid through comparisons to reference plasmids. With this information we proposed an evolutionary horizontal gene transfer (HGT) model for the possible emergence of the pathogen (Brzuszkiewicz et al., 2011). Similarly to ExPEC, E. coli isolates of bovine mastitis are genotypically and phenotypically highly diverse and many studies struggled to determine a positive association of putative VFs. Instead the general E. coli pathogen-associated molecular pattern (PAMP), lipopolysaccharide (LPS), is implicated as a deciding factor for intramammary inflammation. Nevertheless, a mammary pathogenic E. coli (MPEC) pathotype was proposed presumably encompassing strains more adapted to elicit bovine mastitis with virulence traits differentiating them from commensals. We sequenced eight E. coli isolates from udder serous exudate and six fecal commensals (Leimbach et al., 2016). Two mastitis isolate genomes were closed to a finished-grade quality (Leimbach et al., 2015). The genomic sequence of mastitis-associated E. coli (MAEC) strain 1303 was used to elucidate the biosynthesis gene cluster of its O70 LPS O-antigen. We analyzed the phylogenetic genealogy of our strain panel plus eleven bovine-associated E. coli reference strains and found that commensal or MAEC could not be unambiguously allocated to specific phylogroups within a core genome tree of reference E. coli. A thorough gene content analysis could not identify functional convergence of either commensal or MAEC, instead both have only very few gene families enriched in either pathotype. Most importantly, gene content and ecoli_VF_collection analyses showed that no virulence determinants are significantly associated with MAEC in comparison to bovine fecal commensals, disproving the MPEC hypothesis. The genetic repertoire of bovine-associated E. coli, again, is dominated by phylogenetic background. This is also mostly the case for large virulence-associated E. coli gene cluster previously associated with mastitis. Correspondingly, MAEC are facultative and opportunistic pathogens recruited from the bovine commensal gastrointestinal microbiota (Leimbach et al., 2017). Thus, E. coli mastitis should be prevented rather than treated, as antibiotics and vaccines have not proven effective. Although traditional E. coli pathotypes serve a purpose for diagnostics and treatment, it is clear that the current typing system is an oversimplification of E. coli's genomic plasticity. Whole genome sequencing (WGS) revealed many nuances of pathogenic E. coli, including emerging hybrid or heteropathogenic pathotypes. Diagnostic and public health microbiology need to embrace the future by implementing HTS techniques to target patient care and infection control more efficiently. N2 - Eines der definierenden Charakteristika intestinal pathogener E. coli (IPEC) Pathotypen ist ein spezifisches Repertoire an Virulenzfaktoren (VFs). Viele dieser IPEC VFs werden als Typisierungsmarker benutzt. Stattdessen sind Isolate extraintestinal pathogener E. coli (ExPEC) genotypisch vielfältig und beherbergen verschiedenartige VF Sets, welche in der Mehrheit auch als Fitnessfaktoren (FFs) für die gastrointestinale Kolonialisierung fungieren. Das Ziel dieser Dissertation war die genomische Charakterisierung pathogener und kommensaler E. coli in Bezug auf ihren Virulenz- und Antibiotikaresistenz-assoziierten Gengehalt sowie ihre phylogenetische Abstammung. Als Voraussetzung für die vergleichenden Analysen erstellte ich eine E. coli VF-Datenbank, ecoli_VF_collection, mit Fokus auf Virulenz-assoziierte Proteine von ExPEC (Leimbach, 2016b). Darüber hinaus programmierte ich mehrere Skripte und Pipelines zur Anwendung in der bakteriellen Genomik, bac-genomics-scripts (Leimbach, 2016a). Diese Sammlung beinhaltet Tools zur Unterstützung von Assemblierung und Annotation sowie komparativer Genomanalysen, wie Multilokus-Sequenztypisierung (MLST), Zuweisung von Clusters of Orthologous Groups (COG) Kategorien, Suche nach homologen Proteinen, Identifizierung von genomisch unterschiedlichen Regionen (RODs) und Berechnung Pan-genomweiter Assoziationsstatistiken. Mithilfe dieser Tools konnten wir die Prävalenz von 18 Autotransportern (ATs) in einer großen, phylogenetisch heterogenen Stammsammlung bestimmen und nachweisen, dass viele AT-Proteine nicht mit E. coli Pathotypen assoziiert sind. Multivariate Analysen und Statistik legten offen, dass die Verteilung von AT-Varianten vielmehr signifikant von phylogenetischen Abstammungslinien abhängt. Deshalb sind ATs nicht als Marker für Pathotypen geeignet (Zude et al., 2014). Während des bislang größten Ausbruchs von Shiga-Toxin-produzierenden E. coli (STEC) im Jahre 2011 in Deutschland waren wir eines der Teams, welches die genomischen Eigenschaften zweier Isolate analysieren konnte. Basierend auf MLST und Detektion orthologer Proteine zu bekannten E. coli Referenzgenomen konnte ihre enge phylogenetische Verwandschaft und Ähnlichkeit des gesamten Genoms zum enteroaggregativen E. coli (EAEC) 55989 aufgedeckt werden. Im Detail identifizierten wir VFs von STEC und EAEC Pathotypen, vor allem das Prophagen-kodierte Shiga-Toxin (Stx) und ein Plasmid des pAA-Typs kodierend für aggregative Adhärenz-Fimbrien. Die Epidemie wurde demnach durch einen ungewöhnlichen Hybrid-Pathotyp vom O104:H4 Serotyp verursacht. Zusätzlich identifizierten wir die Grundlage für den multiresistenten Phänotyp dieser Ausbruchsstämme auf einem Extended-Spektrum-beta-Laktamase (ESBL) Plasmid über Vergleiche mit Referenzplasmiden. Mit diesen Informationen konnten wir ein horizontales Gentransfer-Modell (HGT) zum Auftreten dieses Pathogenen vorschlagen (Brzuszkiewicz et al., 2011). Ähnlich zu ExPEC sind E. coli Isolate boviner Mastitiden genotypisch und phänotypisch sehr divers, und viele Studien scheiterten am Versuch eine positive Assoziation vermeintlicher VFs nachzuweisen. Stattdessen gilt Lipopolysaccharid (LPS) als entscheidender Faktor zur intramammären Entzündung. Gleichwohl wurde ein mammärer pathogener E. coli (MPEC) Pathotyp vorgeschlagen, der mutmaßlich Stämme umfasst, welche eher geeignet sind eine bovine Mastitis auszulösen und über Virulenz-Merkmale von Kommensalen abgegrenzt werden können. Wir sequenzierten acht E. coli Isolate aus serösem Eutersekret und sechs fäkale Kommensale (Leimbach et al., 2016). Bei zwei Mastitisisolaten wurden die Genome vollständig geschlossen (Leimbach et al., 2015). Anhand der genomischen Sequenz des Mastitis-assoziierten E. coli (MAEC) Stamms 1303 wurde das Gencluster zur Biosynthese seines O70 LPS O-Antigens aufgeklärt. Wir analysierten die phylogenetische Abstammung unserer Stammsammlung plus elf bovin-assoziierter E. coli Referenzstämme, aber konnten weder MAEC noch Kommensale bestimmten Phylogruppen innerhalb eines Core-Genom Stammbaums aus Referenz-E. coli eindeutig zuordnen. Eine ausführliche Gengehalt-Analyse konnte keine funktionelle Konvergenz innerhalb von Kommensalen oder MAEC identifizieren. Stattdessen besitzen beide nur sehr wenige Genfamilien, die bevorzugt in einer der beiden Pathotypen vorkommen. Weder eine Gengehalt- noch eine ecoli_VF_collection-Analyse konnte zeigen, dass eine signifikante Assoziation von bestimmten Virulenzfaktoren mit MAEC, im Vergleich zu bovinen fäkalen Kommensalen, besteht. Damit wurde die MPEC Hypothese widerlegt. Auch das genetische Repertoire von Rinder-assoziierten E. coli wird durch die phylogenetische Abstammung bestimmt. Dies ist überwiegend auch bei großen Virulenz-assoziierten Genclustern der Fall, die bisher mit Mastitis in Verbindung gebracht wurden. Dementsprechend sind MAEC fakultative und opportunistische Pathogene, die ihren Ursprung als Kommensale in der bovinen gastrointestinalen Mikrobiota haben (Leimbach et al., 2017). Obwohl traditionelle E. coli Pathotypen in der Diagnostik und Behandlung einen Zweck erfüllen, ist es offensichtlich, dass das derzeitige Typisierungs-System die genomische Plastizität von E. coli zu sehr vereinfacht. Die Gesamtgenom-Sequenzierung (WGS) deckte viele Nuancen pathogener E. coli auf, einschließlich entstehender hybrider oder heteropathogener Pathotypen. Diagnostische und medizinische Mikrobiologie müssen einen Schritt in Richtung Zukunft gehen und HTS-Technologien anwenden, um Patientenversorgung und Infektionskontrolle effizienter zu unterstützen. KW - Escherichia coli KW - Autotransporter KW - STEC KW - Bovine Mastitis KW - high-throughput sequencing KW - virulence factors KW - pathotypes KW - phylogeny KW - ecoli_VF_collection KW - bac-genomics-scripts KW - autotransporter KW - entero-aggregative-haemorrhagic Escherichia coli (EAHEC) KW - mastitis-associated Escherichia coli (MAEC) Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-154539 ER - TY - JOUR A1 - Oehler, Beatrice A1 - Kistner, Katrin A1 - Martin, Corinna A1 - Schiller, Jürgen A1 - Mayer, Rafaela A1 - Mohammadi, Milad A1 - Sauer, Reine-Solange A1 - Filipovic, Milos R. A1 - Nieto, Francisco R. A1 - Kloka, Jan A1 - Pflücke, Diana A1 - Hill, Kerstin A1 - Schaefer, Michael A1 - Malcangio, Marzia A1 - Reeh, Peter W. A1 - Brack, Alexander A1 - Blum, Robert A1 - Rittner, Heike L. T1 - Inflammatory pain control by blocking oxidized phospholipid-mediated TRP channel activation JF - Scientific Reports N2 - Phospholipids occurring in cell membranes and lipoproteins are converted into oxidized phospholipids (OxPL) by oxidative stress promoting atherosclerotic plaque formation. Here, OxPL were characterized as novel targets in acute and chronic inflammatory pain. Oxidized 1-palmitoyl-2-arachidonoyl-sn-glycero-3-phosphocholine (OxPAPC) and its derivatives were identified in inflamed tissue by mass spectrometry and binding assays. They elicited calcium influx, hyperalgesia and induced pro-nociceptive peptide release. Genetic, pharmacological and mass spectrometric evidence in vivo as well as in vitro confirmed the role of transient receptor potential channels (TRPA1 and TRPV1) as OxPAPC targets. Treatment with the monoclonal antibody E06 or with apolipoprotein A-I mimetic peptide D-4F, capturing OxPAPC in atherosclerosis, prevented inflammatory hyperalgesia, and in vitro TRPA1 activation. Administration of D-4F or E06 to rats profoundly ameliorated mechanical hyperalgesia and inflammation in collagen-induced arthritis. These data reveal a clinically relevant role for OxPAPC in inflammation offering therapy for acute and chronic inflammatory pain treatment by scavenging OxPAPC. KW - chronic pain KW - ion channels in the nervous system KW - molecular medicine KW - pain Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-158536 VL - 7 IS - 5447 ER - TY - JOUR A1 - Wallmann-Sperlich, Birgit A1 - Bipp, Tanja A1 - Bucksch, Jens A1 - Froboese, Ingo T1 - Who uses height-adjustable desks? - Sociodemographic, health-related, and psycho-social variables of regular users JF - International Journal of Behavioral Nutrition and Physical Activity N2 - Background: Sit-to-stand height-adjustable desks (HAD) may promote workplace standing, as long as workers use them on a regular basis. The aim of this study was to investigate (i) how common HAD in German desk-based workers are, and how frequently HADs are used, (ii) to identify sociodemographic, health-related, and psycho-social variables of workday sitting including having a HAD, and (iii) to analyse sociodemographic, health-related, and psycho-social variables of users and non-users of HADs. Methods: A cross-sectional sample of 680 participants (51.9% men; 41.0 ± 13.1 years) in a desk-based occupation was interviewed by telephone about their occupational sitting and standing proportions, having and usage of a HAD, and answered questions concerning psycho-social variables of occupational sitting. The proportion of workday sitting was calculated for participants having an HAD (n = 108) and not-having an HAD (n = 573), as well as for regular users of HAD (n = 54), and irregular/non-users of HAD (n = 54). Linear regressions were conducted to calculate associations between socio-demographic, health-related, psychosocial variables and having/not having an HAD, and the proportion of workday sitting. Logistic regressions were executed to examine the association of mentioned variables and participants’ usage of HADs. Results: Sixteen percent report that they have an HAD, and 50% of these report regular use of HAD. Having an HAD is not a correlate of the proportion of workday sitting. Further analysis restricted to participants having available a HAD highlights that only the ‘perceived advantages of sitting less’ was significantly associated with HAD use in the fully adjusted model (OR 1.75 [1.09; 2.81], p < 0.05). Conclusions: The present findings indicate that accompanying behavioral action while providing an HAD is promising to increase the regular usage of HAD. Hence, future research needs to address the specificity of behavioral actions in order to enhance regular HAD use, and needs to give more fundamental insights into these associations. KW - cross-sectional KW - office-workers KW - desk-based KW - height-adjustable desk KW - occupational sitting and physical activity questionnaire KW - sitting time KW - correlates KW - natural approach Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-157888 VL - 14 IS - 26 ER - TY - JOUR A1 - Scheiner, Ricarda A1 - Entler, Brian V. A1 - Barron, Andrew B. A1 - Scholl, Christina A1 - Thamm, Markus T1 - The Effects of Fat Body Tyramine Level on Gustatory Responsiveness of Honeybees (Apis mellifera) Differ between Behavioral Castes JF - Frontiers in Systems Neuroscience N2 - Division of labor is a hallmark of social insects. In the honeybee (Apis mellifera) each sterile female worker performs a series of social tasks. The most drastic changes in behavior occur when a nurse bee, who takes care of the brood and the queen in the hive, transitions to foraging behavior. Foragers provision the colony with pollen, nectar or water. Nurse bees and foragers differ in numerous behaviors, including responsiveness to gustatory stimuli. Differences in gustatory responsiveness, in turn, might be involved in regulating division of labor through differential sensory response thresholds. Biogenic amines are important modulators of behavior. Tyramine and octopamine have been shown to increase gustatory responsiveness in honeybees when injected into the thorax, thereby possibly triggering social organization. So far, most of the experiments investigating the role of amines on gustatory responsiveness have focused on the brain. The potential role of the fat body in regulating sensory responsiveness and division of labor has large been neglected. We here investigated the role of the fat body in modulating gustatory responsiveness through tyramine signaling in different social roles of honeybees. We quantified levels of tyramine, tyramine receptor gene expression and the effect of elevating fat body tyramine titers on gustatory responsiveness in both nurse bees and foragers. Our data suggest that elevating the tyramine titer in the fat body pharmacologically increases gustatory responsiveness in foragers, but not in nurse bees. This differential effect of tyramine on gustatory responsiveness correlates with a higher natural gustatory responsiveness of foragers, with a higher tyramine receptor (Amtar1) mRNA expression in fat bodies of foragers and with lower baseline tyramine titers in fat bodies of foragers compared to those of nurse bees. We suggest that differential tyramine signaling in the fat body has an important role in the plasticity of division of labor through changing gustatory responsiveness. KW - behavior KW - biogenic amines KW - division of labor KW - nurse bee KW - forager KW - PER KW - octopamine KW - insect Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-157874 VL - 11 IS - 55 ER - TY - JOUR A1 - Lamaze, Angelique A1 - Öztürk-Çolak, Arzu A1 - Fischer, Robin A1 - Peschel, Nicolai A1 - Koh, Kyunghee A1 - Jepson, James E. C. T1 - Regulation of sleep plasticity by a thermo-sensitive circuit in Drosophila JF - Scientific Reports N2 - Sleep is a highly conserved and essential behaviour in many species, including the fruit fly Drosophila melanogaster. In the wild, sensory signalling encoding environmental information must be integrated with sleep drive to ensure that sleep is not initiated during detrimental conditions. However, the molecular and circuit mechanisms by which sleep timing is modulated by the environment are unclear. Here we introduce a novel behavioural paradigm to study this issue. We show that in male fruit flies, onset of the daytime siesta is delayed by ambient temperatures above 29°C. We term this effect Prolonged Morning Wakefulness (PMW). We show that signalling through the TrpA1 thermo-sensor is required for PMW, and that TrpA1 specifically impacts siesta onset, but not night sleep onset, in response to elevated temperatures. We identify two critical TrpA1-expressing circuits and show that both contact DN1p clock neurons, the output of which is also required for PMW. Finally, we identify the circadian blue-light photoreceptor CRYPTOCHROME as a molecular regulator of PMW, and propose a model in which the Drosophila nervous system integrates information encoding temperature, light, and time to dynamically control when sleep is initiated. Our results provide a platform to investigate how environmental inputs co-ordinately regulate sleep plasticity. KW - Circadian rhythms and sleep KW - Genetics KW - Drosophila melanogaster Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-181146 VL - 7 ER - TY - JOUR A1 - Ruppert, Manuela A1 - Franz, Mirjam A1 - Saratis, Anastasios A1 - Escarcena, Laura Velo A1 - Hendrich, Oliver A1 - Gooi, Li Ming A1 - Schwenkert, Isabell A1 - Klebes, Ansgar A1 - Scholz, Henrike T1 - Hangover links nuclear RNA signaling to cAMP regulation via the phosphodiesterase 4d ortholog dunce JF - Cell Reports N2 - The hangover gene defines a cellular stress pathway that is required for rapid ethanol tolerance in Drosophila melanogaster. To understand how cellular stress changes neuronal function, we analyzed Hangover function on a cellular and neuronal level. We provide evidence that Hangover acts as a nuclear RNA binding protein and we identified the phosphodiesterase 4d ortholog dunce as a target RNA. We generated a transcript-specific dunce mutant that is impaired not only in ethanol tolerance but also in the cellular stress response. At the neuronal level, Dunce and Hangover are required in the same neuron pair to regulate experience-dependent motor output. Within these neurons, two cyclic AMP (cAMP)-dependent mechanisms balance the degree of tolerance. The balance is achieved by feedback regulation of Hangover and dunce transcript levels. This study provides insight into how nuclear Hangover/RNA signaling is linked to the cytoplasmic regulation of cAMP levels and results in neuronal adaptation and behavioral changes. KW - biology KW - hangover KW - dunce KW - Dunce isoforms KW - PDE4d KW - cellular stress KW - alcohol tolerance KW - Drosophila melanogaster Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-171950 VL - 18 IS - 2 ER - TY - JOUR A1 - Ewald, Jan A1 - Bartl, Martin A1 - Dandekar, Thomas A1 - Kaleta, Christoph T1 - Optimality principles reveal a complex interplay of intermediate toxicity and kinetic efficiency in the regulation of prokaryotic metabolism JF - PLOS Computational Biology N2 - A precise and rapid adjustment of fluxes through metabolic pathways is crucial for organisms to prevail in changing environmental conditions. Based on this reasoning, many guiding principles that govern the evolution of metabolic networks and their regulation have been uncovered. To this end, methods from dynamic optimization are ideally suited since they allow to uncover optimality principles behind the regulation of metabolic networks. We used dynamic optimization to investigate the influence of toxic intermediates in connection with the efficiency of enzymes on the regulation of a linear metabolic pathway. Our results predict that transcriptional regulation favors the control of highly efficient enzymes with less toxic upstream intermediates to reduce accumulation of toxic downstream intermediates. We show that the derived optimality principles hold by the analysis of the interplay between intermediate toxicity and pathway regulation in the metabolic pathways of over 5000 sequenced prokaryotes. Moreover, using the lipopolysaccharide biosynthesis in Escherichia coli as an example, we show how knowledge about the relation of regulation, kinetic efficiency and intermediate toxicity can be used to identify drug targets, which control endogenous toxic metabolites and prevent microbial growth. Beyond prokaryotes, we discuss the potential of our findings for the development of antifungal drugs. KW - Enzyme regulation KW - Toxicity KW - Metabolic pathways KW - Enzymes KW - Transcriptional control KW - Enzyme kinetics KW - Enzyme metabolism KW - Predictive toxicology Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-180870 VL - 13 IS - 2 ER - TY - JOUR A1 - Van Steenbergen, Anne A1 - Balteau, Magali A1 - Ginion, Audrey A1 - Ferté, Laura A1 - Battault, Sylvain A1 - de Meester de Ravenstein, Christophe A1 - Balligand, Jean-Luc A1 - Daskalopoulos, Evangelos-Panagiotis A1 - Gilon, Patrick A1 - Despa, Florin A1 - Despa, Sanda A1 - Vanoverschelde, Jean-Louis A1 - Horman, Sandrine A1 - Koepsell, Hermann A1 - Berry, Gerard A1 - Hue, Louis A1 - Bertrand, Luc A1 - Beauloye, Christophe T1 - Sodium-myoinositol cotransporter-1, SMIT1, mediates the production of reactive oxygen species induced by hyperglycemia in the heart JF - Scientific Reports N2 - Hyperglycemia (HG) stimulates the production of reactive oxygen species in the heart through activation of NADPH oxidase 2 (NOX2). This production is independent of glucose metabolism but requires sodium/glucose cotransporters (SGLT). Seven SGLT isoforms (SGLT1 to 6 and sodium-myoinositol cotransporter-1, SMIT1) are known, although their expression and function in the heart remain elusive. We investigated these 7 isoforms and found that only SGLT1 and SMIT1 were expressed in mouse, rat and human hearts. In cardiomyocytes, galactose (transported through SGLT1) did not activate NOX2. Accordingly, SGLT1 deficiency did not prevent HG-induced NOX2 activation, ruling it out in the cellular response to HG. In contrast, myo-inositol (transported through SMIT1) reproduced the toxic effects of HG. SMIT1 overexpression exacerbated glucotoxicity and sensitized cardiomyocytes to HG, whereas its deletion prevented HG-induced NOX2 activation. In conclusion, our results show that heart SMIT1 senses HG and triggers NOX2 activation. This could participate in the redox signaling in hyperglycemic heart and contribute to the pathophysiology of diabetic cardiomyopathy. KW - hyperglycemia KW - Sodium-myoinositol cotransporter-1 (SMIT1) KW - glucose metabolism KW - heart KW - NADPH oxidase 2 (NOX2) KW - sodium/glucose cotransporters (SGLT) KW - cardiomyocytes Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-180891 VL - 7 ER - TY - JOUR A1 - Adrián-Martínez, S. A1 - Albert, A. A1 - André, M. A1 - Anghinolfi, M. A1 - Anton, G. A1 - Ardid, M. A1 - Aubert, J.-J. A1 - Baret, B. A1 - Barrios-Marti, J. A1 - Basa, S. A1 - Bertin, V. A1 - Biagi, S. A1 - Bormuth, R. A1 - Bouwhuis, M.C. A1 - Bruijn, R. A1 - Brunner, J. A1 - Buto, J. A1 - Capone, A. A1 - Caramete, L. A1 - Carr, J. A1 - Chiarusi, T. A1 - Circella, M. A1 - Coniglione, R. A1 - Costantini, H. A1 - Coyle, P. A1 - Creusot, A. A1 - Dekeyser, I. A1 - Deschamps, A. A1 - De Bonis, G. A1 - Distefano, C. T1 - Stacked search for time shifted high energy neutrinos from gamma ray bursts with the ANTARES neutrino telescope JF - European Physical Journal C N2 - A search for high-energy neutrino emission correlated with gamma-ray bursts outside the electromagnetic prompt-emission time window is presented. Using a stacking approach of the time delays between reported gamma-ray burst alerts and spatially coincident muon-neutrino signatures, data from the Antares neutrino telescope recorded between 2007 and 2012 are analysed. One year of public data from the IceCube detector between 2008 and 2009 have been also investigated. The respective timing profiles are scanned for statistically significant accumulations within 40 days of the Gamma Ray Burst, as expected from Lorentz Invariance Violation effects and some astrophysical models. No significant excess over the expected accidental coincidence rate could be found in either of the two data sets. The average strength of the neutrino signal is found to be fainter than one detectable neutrino signal per hundred gamma-ray bursts in the Antares data at 90% confidence level. KW - Search window KW - Neutrino data KW - Neutrino telescope KW - Neutrino emission KW - Accidental coincidence KW - Gamma-ray bursts Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-181251 VL - 77 IS - 1 ER -