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Titlebook: Bacteria and Complement; Michael Loos Book 1985 The Editor(s) (if applicable) and The Author(s), under exclusive license to Springer-Verla

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Evidence for Direct Binding of the First Component of Complement, C1, to Outer Membrane Proteins frtion of proteins in the outer membrane is also indicated by the fact that various major outer membrane proteins in association with LPS, serve as receptors for phages (Datta et al. 1977; Mu-TOH et al. 1978; . and . 1979; . and . 1982) and colicins (. et al. 1979; . 1979).
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Mathematics and Its Applicationsy, I (C3b inactivator or C3b INA) and H (β1 or C3b INA accelerator) for the alternative pathway, and anaphylatoxin inactivator. Due to the dramatic advances in protein chemistry, these 19 distinct serum proteins have been highly purified and characterized physiochemically (Table 1).
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Development of Stability Indicating Methodsellular bacteria which are resistant to intracellular killing unless macrophages are activated. Humoral immune mechanisms (antibody, complement) deal mainly with extracellular bacteria, while cellular immune mechanisms (T cells, macrophages) deal with facultative intracellular bacteria (. 1983).
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https://doi.org/10.1007/978-0-387-85627-8on and biological consequences of complement deposition and complement activation by pathogenic gram-negative bacteria. The purpose of this chapter is to provide a brief review of existing data in these areas and to outline in detail the work done in our laboratory over the last 4 years on complement activation by gramnegative bacteria.
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Differences in Attachment and Phagocytosis of , Strains (S Form, Re Mutant) by Mouse Peritoneal Macellular bacteria which are resistant to intracellular killing unless macrophages are activated. Humoral immune mechanisms (antibody, complement) deal mainly with extracellular bacteria, while cellular immune mechanisms (T cells, macrophages) deal with facultative intracellular bacteria (. 1983).
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Studies on the Mechanism of Bacterial Resistance to Complement-Mediated Killing and on the Mechanison and biological consequences of complement deposition and complement activation by pathogenic gram-negative bacteria. The purpose of this chapter is to provide a brief review of existing data in these areas and to outline in detail the work done in our laboratory over the last 4 years on complement activation by gramnegative bacteria.
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