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Titlebook: Bacterial Protein Toxins; Klaus Aktories,Ingo Just Book 2000 Springer-Verlag Berlin Heidelberg 2000 Antigen.Eiweiss.Gift.bacterial protein

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Ideologie, Hegemonie und Diskurstic targeting approaches, such as antisense-oligonucleotide strategies or the gene-“knock-out” technology, PT is appreciated as a valuable tool in cell biology for discovering novel G-protein-coupled signaling pathways (. 1998; . 1998).
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Pertussis Toxin as a Pharmacological Tool,tic targeting approaches, such as antisense-oligonucleotide strategies or the gene-“knock-out” technology, PT is appreciated as a valuable tool in cell biology for discovering novel G-protein-coupled signaling pathways (. 1998; . 1998).
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Structure and Function of Actin-Adenosine-Diphosphate-Ribosylating Toxins,cus on research on these new bacterial toxins, especially on the molecular structures and functions of the clostridial actin-specific ADP-ribosylating toxins. To date, the actin-specific ADP-ribosylating toxins elaborated by the bacteria other than clostridia have not yet been explored.
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Anthrax Toxin,imals from infection (. 1946) demonstrates that anthrax, like diphtheria and tetanus, is a strongly toxin-dependent disease. .-type . strains lacking pXO2 are effective live vaccines, because they are avirulent but still able to make toxin and induce anti-toxin antibodies (. 1937).
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0171-2004 tein toxins. This refers especially to structural aspects of protein toxins but also holds true for genetics, molecular biology and biochemical mechanisms underlying the action of toxins. This volume covers the very current and exciting aspects of up-to-date bacterial toxicology and comprehensively
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Verfahren des Werbemittel-Pretestingg demonstrated to have intracellular sites of action. This implies that the toxins must be able to cross cellular membranes. Most toxins do this by crossing membranes of intracellular organelles rather than penetrating the plasma membrane.
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Justin Becker,Volker Trommsdorffino acid of the substrate molecule, which is usually forced to undergo a functional change (Fig. 1). When the reaction is mediated by a toxin, this event ultimately results in either malfunction or death of the target eukaryotic cells.
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