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Second Edition of the German–Austrian S3 Guideline “Infarction-related cardiogenic shock: diagnosis, monitoring and treatment” (2024)
Pilarczyk, Kevin ; Boeken, Udo ; Russ, Martin ; Briegel, Josef ; Buerke, Michael ; Geppert, Alexander ; Janssens, Uwe ; Kelm, Malte ; Michels, Guido ; Schlitt, Axel ; Thiele, Holger ; Willems, Stephan ; Zeymer, Uwe ; Zwissler, Bernhard ; Delle-Karth, Georg ; Ferrari, Markus Wolfgang ; Figulla, Hans Reiner ; Heller, Axel R. ; Hindricks, Gerhard ; Pichler-Cetin, Emel ; Pieske, Burkert ; Prondzinsky, Roland ; Bauersachs, Johann ; Kopp, Ina ; Werdan, Karl ; Thielmann, Matthias
Depinning of three-dimensional drops from wettability defects (2009)
Beltrame, Philippe ; Hänggi, Peter ; Thiele, Uwe
Rayleigh and depinning instabilities of forced liquid ridges on heterogeneous substrates (2011)
Beltrame, Philippe ; Knobloch, Edgar ; Hänggi, Peter ; Thiele, Uwe
Depinning of 2d and 3d droplets blocked by a hydrophobic defect (2010)
Beltrame, Philippe ; Hänggi, Peter ; Knobloch, E. ; Thiele, Uwe
Ratchet-driven fluid transport in bounded two-layer films of immiscible liquids (2008)
John, Karin ; Hänggi, Peter ; Thiele, Uwe
Benchmarking whole exome sequencing in the German network for personalized medicine (2024)
Menzel, Michael ; Martis-Thiele, Mihaela ; Goldschmid, Hannah ; Ott, Alexander ; Romanovsky, Eva ; Siemanowski-Hrach, Janna ; Seillier, Lancelot ; Ortiz Brüchle, Nadina ; Maurer, Angela ; Lehmann, Kjong-Van ; Begemann, Matthias ; Elbracht, Miriam ; Meyer, Robert ; Dintner, Sebastian ; Claus, Rainer ; Meier-Kolthoff, Jan ; Blanc, Eric ; Möbs, Markus ; Joosten, Maria ; Benary, Manuela ; Basitta, Patrick ; Hölscher, Florian ; Tischler, Verena ; Groß, Thomas ; Kutz, Oliver ; Prause, Rebecca ; William, Doreen ; Horny, Kai ; Goering, Wolfgang ; Sivalingam, Sugirthan ; Borkhardt, Arndt ; Blank, Cornelia ; Junk, Stefanie ; Yasin, Layal ; Moskalev, Evgeny A. ; Carta, Maria Giulia ; Ferrazzi, Fulvia ; Tögel, Lars ; Wolter, Steffen ; Adam, Eugen ; Matysiak, Uta ; Rosenthal, Tessa ; Dönitz, Jürgen ; Lehmann, Ulrich ; Schmidt, Gunnar ; Bartels, Stephan ; Hofmann, Winfried ; Hirsch, Steffen ; Dikow, Nicola ; Göbel, Kirsten ; Banan, Rouzbeh ; Hamelmann, Stefan ; Fink, Annette ; Ball, Markus ; Neumann, Olaf ; Rehker, Jan ; Kloth, Michael ; Murtagh, Justin ; Hartmann, Nils ; Jurmeister, Phillip ; Mock, Andreas ; Kumbrink, Jörg ; Jung, Andreas ; Mayr, Eva-Maria ; Jacob, Anne ; Trautmann, Marcel ; Kirmse, Santina ; Falkenberg, Kim ; Ruckert, Christian ; Hirsch, Daniela ; Immel, Alexander ; Dietmaier, Wolfgang ; Haack, Tobias ; Marienfeld, Ralf ; Fürstberger, Axel ; Niewöhner, Jakob ; Gerstenmaier, Uwe ; Eberhardt, Timo ; Greif, Phillip ; Appenzeller, Silke ; Maurus, Katja ; Doll, Julia ; Jelting, Yvonne ; Jonigk, Danny ; Märkl, Bruno ; Beule, Dieter ; Horst, David ; Wulf, Anna-Lena ; Aust, Daniela ; Werner, Martin ; Reuter-Jessen, Kirsten ; Ströbel, Philipp ; Auber, Bernd ; Sahm, Felix ; Merkelbach-Bruse, Sabine ; Siebolts, Udo ; Roth, Wilfried ; Lassmann, Silke ; Klauschen, Frederick ; Gaisa, Nadine T. ; Weichert, Wilko ; Evert, Matthias ; Armeanu-Ebinger, Sorin ; Ossowski, Stephan ; Schroeder, Christopher ; Schaaf, Christian P. ; Malek, Nisar ; Schirmacher, Peter ; Kazdal, Daniel ; Pfarr, Nicole ; Budczies, Jan ; Stenzinger, Albrecht
Introduction Whole Exome Sequencing (WES) has emerged as an efficient tool in clinical cancer diagnostics to broaden the scope from panel-based diagnostics to screening of all genes and enabling robust determination of complex biomarkers in a single analysis. Methods To assess concordance, six formalin-fixed paraffin-embedded (FFPE) tissue specimens and four commercial reference standards were analyzed by WES as matched tumor-normal DNA at 21 NGS centers in Germany, each employing local wet-lab and bioinformatics investigating somatic and germline variants, copy-number alteration (CNA), and different complex biomarkers. Somatic variant calling was performed in 494 diagnostically relevant cancer genes. In addition, all raw data were re-analyzed with a central bioinformatic pipeline to separate wet- and dry-lab variability. Results The mean positive percentage agreement (PPA) of somatic variant calling was 76% and positive predictive value (PPV) 89% compared a consensus list of variants found by at least five centers. Variant filtering was identified as the main cause for divergent variant calls. Adjusting filter criteria and re-analysis increased the PPA to 88% for all and 97% for clinically relevant variants. CNA calls were concordant for 82% of genomic regions. Calls of homologous recombination deficiency (HRD), tumor mutational burden (TMB), and microsatellite instability (MSI) status were concordant for 94%, 93%, and 93% respectively. Variability of CNAs and complex biomarkers did not increase considerably using the central pipeline and was hence attributed to wet-lab differences. Conclusion Continuous optimization of bioinformatic workflows and participating in round robin tests are recommend.
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