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Literature DB >> 3552987

Stimulation of complement component C3 synthesis in macrophagelike cell lines by group B streptococci.

Abstract

Complement levels and complement activation are key determinants in streptococcus-induced inflammatory responses. Activation of macrophage functions, such as complement synthesis, by group B streptococci (GBS) was examined as a possible component of GBS-induced chronic inflammation. Using an enzyme-linked immunosorbent assay, secreted C3 from mouse macrophagelike cell lines (PU5-1.8 and J774A.1) was monitored after cultivation with GBS. Whole, heat-killed GBS (1 to 10 CFU per macrophage) of both type Ia and III strains induced 25 to 300% increases in secreted C3 in both cell lines after a 24-h cultivation. GBS-treated cell lines exhibited increases in secreted lysozyme (10%) and in cellular protein (25 to 50%). Inhibition of macrophage phagocytosis by cytochalasin B inhibited GBS stimulation of C3. Purified cell walls of GBS type III strain 603-79 (1 to 10 micrograms/ml) also enhanced C3 synthesis. Local enhancement of macrophage C3 production by ingested streptococci or by persistent cell wall antigens may serve to promote chronic inflammatory responses.

Entities: Chemical Disease Species

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Year: 1987 PMID： 3552987 PMCID： PMC260475 DOI： 10.1128/iai.55.5.1101-1105.1987

Source DB: PubMed Journal: Infect Immun ISSN： 0019-9567 Impact factor: 3.441

34 in total

Review 1. The macrophage as a secretory cell.

Authors: R C Page; P Davies; A C Allison
Journal: Int Rev Cytol Date: 1978

Review 2. Synthesis and secretion of complement proteins by macrophages.

Authors: H R Colten; Y M Ooi; P J Edelson
Journal: Ann N Y Acad Sci Date: 1979 Impact factor: 5.691

3. Antibody-independent activation of C1 by type Ia group B streptococci.

Authors: M E Eads; N J Levy; D L Kasper; C J Baker; A Nicholson-Weller
Journal: J Infect Dis Date: 1982-11 Impact factor: 5.226

4. In vivo changes in complement induced with peptidoglycan-polysaccharide polymers from streptococcal cell walls.

Authors: J D Lambris; J B Allen; J H Schwab
Journal: Infect Immun Date: 1982-01 Impact factor: 3.441

5. Studies on group B beta-hemolytic Streptococcus. I. Isolation and partial characterization of an extracellular toxin.

Authors: C G Hellerqvist; J Rojas; R S Green; S Sell; H Sundell; M T Stahlman
Journal: Pediatr Res Date: 1981-06 Impact factor: 3.756

6. Studies on the possible involvement of complement component C3 in the initiation of acid hydrolase secretion by macrophages. I. Correlation between enzyme-releasing and complement-activating capacities of several secretagogues.

Authors: D W Riches; D R Stanworth
Journal: Immunology Date: 1981-09 Impact factor: 7.397

7. Quantitative studies of the secretion of complement component C3 by resident, elicited and activated macrophages. Comparison with C2, C4 and lysosomal enzyme release.

Authors: B Zimmer; H P Hartung; G Scharfenberger; D Bitter-Suermann; U Hadding
Journal: Eur J Immunol Date: 1982-05 Impact factor: 5.532

4. Increased C3 production in human monocytes after stimulation with Candida albicans is suppressed by granulocyte-macrophage colony-stimulating factor.

Authors: A K Høgåsen; T G Abrahamsen
Journal: Infect Immun Date: 1993-05 Impact factor: 3.441

5. Polymyxin B stimulates production of complement components and cytokines in human monocytes.

Authors: A K Høgåsen; T G Abrahamsen
Journal: Antimicrob Agents Chemother Date: 1995-02 Impact factor: 5.191

5 in total

Stimulation of complement component C3 synthesis in macrophagelike cell lines by group B streptococci.

Review 1. The macrophage as a secretory cell.

Review 2. Synthesis and secretion of complement proteins by macrophages.

3. Antibody-independent activation of C1 by type Ia group B streptococci.

4. In vivo changes in complement induced with peptidoglycan-polysaccharide polymers from streptococcal cell walls.

5. Studies on group B beta-hemolytic Streptococcus. I. Isolation and partial characterization of an extracellular toxin.

6. Studies on the possible involvement of complement component C3 in the initiation of acid hydrolase secretion by macrophages. I. Correlation between enzyme-releasing and complement-activating capacities of several secretagogues.

7. Quantitative studies of the secretion of complement component C3 by resident, elicited and activated macrophages. Comparison with C2, C4 and lysosomal enzyme release.

8. Processing of streptococcal cell walls by rat macrophages and human monocytes in vitro.

9. Rat arthritis due to whole group B streptococci. Clinical and histopathologic features compared with groups A and D.

10. Arthritis in rats after systemic injection of streptococcal cells or cell walls.

1. Secretion of the C3 component of complement by peritoneal cells cultured with encapsulated Cryptococcus neoformans.

2. Entry and intracellular survival of group B streptococci in J774 macrophages.

3. Opsonin-independent phagocytosis of group B streptococci: role of complement receptor type three.

4. Increased C3 production in human monocytes after stimulation with Candida albicans is suppressed by granulocyte-macrophage colony-stimulating factor.

5. Polymyxin B stimulates production of complement components and cytokines in human monocytes.