Versuch einer theologischen Neuinterpretation des Fußbodenmosaiks der Memorialkirche in Teurnia

Die frühchristliche Memorialkirche von Teurnia wurde 1908 bei Wasserleitungsbauarbeiten entdeckt, in der südlichen Seitenkapelle befindet sich jenes Mosaik, welches Gegenstand dieser Arbeit ist. Seit der Entdeckung des Mosaiks ist die Diskussion über die Möglichkeiten seiner Interpretation nicht abgerissen und doch gibt es eine, auf J. Hagenauer zurückgehende, die sich anscheinend durchgesetzt hat. Diese Arbeit versucht eine andere mögliche Deutung des Mosaiks aufzuzeigen. Besonderes Augenmerk ist auf den Prozess der Christianisierung zu legen, der sich im Übergang von der Antike zum Mittelalter vollzieht. Es wird gefragt inwiefern sich die Religiosität der Menschen veränderte und was das übergeordnete Thema des Mosaiks ist. Der Versuch einer Neuinterpretation wird getragen von den drei folgenden kulturwissenschaftlichen Bezeichnungen für solche Prozesse: Akkulturation, Enkulturation und Inkulturation. Die Metafrage der bei dieser Arbeit nachgegangen werden soll lautet demnach: Ist das Fußbodenmosaik zu verstehen im Rahmen eines Akkulturations-, Enkulturations- oder Inkulturationsvorganges

Prognostic significance of endogenous adhesion/growth-regulatory lectins in lung cancer

Objective: To determine the expression of endogenous adhesion/growth-regulatory lectins and their binding sites using labeled tissue lectins as well as the binding profile of hyaluronic acid as an approach to define new prognostic markers. Methods: Sections of paraffin-embedded histological material of 481 lungs from lung tumor patients following radical lung excision processed by a routine immunohistochemical method (avidin-biotin labeling, DAB chromogen). Specific antibodies against galectins-1 and - 3 and the heparin-binding lectin were tested. Staining by labeled galectins and hyaluronic acid was similarly visualized by a routine protocol. After semiquantitative assessment of staining, the results were compared with the pT and pN stages and the histological type. Survival was calculated by univariate and multivariate methods. Results: Binding of galectin-1 and its expression tended to increase, whereas the parameters for galectin-3 decreased in advanced pT and pN stages at a statistically significant level. The number of positive cases was considerably smaller among the cases with small cell lung cancer than in the group with non-small-cell lung cancer, among which adenocarcinomas figured prominently with the exception of galectin-1 expression. Kaplan-Meier computations revealed that the survival rate of patients with galectin-3-binding or galectin-1-expressing tumors was significantly poorer than that of the negative cases. In the multivariate calculations of survival lymph node metastases ( p < 0.0001), histological type ( p = 0.003), galectin-3-binding capacity ( p = 0.01), galectin-3 expression ( p = 0.03) and pT status ( p = 0.003) proved to be independent prognostic factors, not correlated with the pN stage. Conclusion: The expression and the capacity to bind the adhesion/growth regulatory galectin-3 is defined as an unfavorable prognostic factor not correlated with the pTN stage. Copyright (C) 2005 S. Karger AG, Basel

Enhanced Membrane Pore Formation through High-Affinity Targeted Antimicrobial Peptides

Many cationic antimicrobial peptides (AMPs) target the unique lipid composition of the prokaryotic cell membrane. However, the micromolar activities common for these peptides are considered weak in comparison to nisin, which follows a targeted, pore-forming mode of action. Here we show that AMPs can be modified with a high-affinity targeting module, which enables membrane permeabilization at low concentration. Magainin 2 and a truncated peptide analog were conjugated to vancomycin using click chemistry, and could be directed towards specific membrane embedded receptors both in model membrane systems and whole cells. Compared with untargeted vesicles, a gain in permeabilization efficacy of two orders of magnitude was reached with large unilamellar vesicles that included lipid II, the target of vancomycin. The truncated vancomycin-peptide conjugate showed an increased activity against vancomycin resistant Enterococci, whereas the full-length conjugate was more active against a targeted eukaryotic cell model: lipid II containing erythrocytes. This study highlights that AMPs can be made more selective and more potent against biological membranes that contain structures that can be targeted

Synthesis of bicyclic tripeptides inspired by the ABC-ring system of vancomycin through ruthenium-based cyclization chemistries

The synthesis of a bicyclic tripeptide that mimics the ABC ring system of vancomycin is described by using a ring closing metathesis (RCM) – peptide coupling – ruthenium-catalyzed azide-alkyne cycloaddition (RuAAC) strategy