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SFB 617:  Molecular mechanisms of epithelial defense

Subject Area Biology
Term from 2002 to 2009
Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 5485085
 
It is the aim of the collaborative research centre to investigate, why healthy body surfaces - despite the continous presence of potentially pathogenic microorganisms - usually are not infected and how epithelia actively defend infection-independent from specialized leukocytes of the immune system. One focus will be on microbicidal peptides and proteins of different epithelial origin. In particular, we will analyse such peptides obtained from the invertebrate Hydra, from human origin (from human skin, the gastrointestinal tract and the lung), from cow skin as well as from mouse skin. Both, constitutively produced antimicrobial peptides, which act against a more or less restricted spectrum of microorganisms, and other, by contact of epithelial cells with pathogens induced antimicrobial peptides, will be analysed. Furthermore, by pathogens produced inducers of antimicrobial peptides in epithelial cells and factors that cleave inactive precursors of epithelial peptide antibiotics to generate active forms as well as microbial factors that induce production of proinflammatory cytokines in epithelial cells, will be structurally characterised. We will analyse, which peptide antibiotics are induced by these "pathogen-associated molecules" in different epithelia. Furthermore, by recombinant techniques generated antimicrobial peptides will be investigated for their biophysical and physico-biochemical properties to get an idea about the mode of action of these peptides in microbial killing. We hope to get progress in understanding the strategy, how healthy epithelia keep healthy. Our findings should give new ideas in understanding the pathophysiology of locally occuring recurrent infections, in particular in the skin, the gut, the genito-urinary tract and the lung. A major aim of our project will be also to present basic knowledge to generate a new generation of antibiotics, which, due to its completely different mode of action, could represent future alternatives to fight against pathogens that are resistant towards classical antibiotics. Search for inducible peptide antibiotics and the discovery of pathogen-associated molecules that induce petide antibiotics, but not proinflammatory cytokines, should allow new concepts of "immune stimulation" of the epithelial innate immune system.
DFG Programme Collaborative Research Centres

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