Your search keyword '"Warejcka DJ"' showing total 2 results

1. Toxicity of group B Streptococcus agalactiae in adult rats.

Author

Warejcka DJ, Goodrum KJ, and Spitznagel JK

Subjects

Animals, Complement C3 analysis, Female, Fibrinogen analysis, Hemoglobinuria etiology, Hemolysis, Hemorrhage etiology, Kidney pathology, Leukocyte Count, Liver pathology, Lung pathology, Platelet Count, Rats, Rats, Inbred Strains, Spleen pathology, Bacterial Toxins toxicity, Streptococcus agalactiae pathogenicity

Abstract

Several strains of group B Streptococcus agalactiae were found to be lethal for young adult rats. When bacteria were heat killed and then injected intraperitoneally into rats, rapid death (14 to 18 h) of the rats occurred, characterized by labored breathing, hemolyzed serum, hemoglobinuria, and subungual hemorrhages. Sections of tissues from these rats failed to reveal the cause of death. Rats injected with toxic or nontoxic strains of group B S. agalactiae had reduced numbers of circulating leukocytes and low serum C3 levels in comparison with those in control rats. The toxic strains of group B S. agalactiae induced dramatic decreases in platelet numbers, and in plasma fibrinogen levels as well, suggesting that the toxicity was due to disruption of the coagulation system. Rapid death in the absence of infection suggests that group B S. agalactiae may have a cell-associated toxin that induces these changes. Such a toxin may be a contributory factor in the high mortality rate associated with group B streptococcal infections of the human neonate.

Published

1985

2. Modulation of complement fixation and the phlogistic capacity of group A, B, and D streptococci by human lysozyme acting on their cell walls.

Author

Spitznagel JK, Goodrum KJ, Warejcka DJ, Weaver JL, Miller HL, and Babcock L

Subjects

Animals, Cell Wall immunology, Cell Wall metabolism, Chemotactic Factors metabolism, Complement Fixation Tests, Endopeptidases metabolism, Enterococcus faecalis immunology, Humans, Inflammation immunology, Neuraminidase metabolism, Polysaccharides, Bacterial immunology, Rats, Streptococcus agalactiae immunology, Streptococcus pyogenes immunology, Complement Activation, Complement Pathway, Alternative, Muramidase metabolism, Streptococcus immunology

Abstract

Streptococci and streptococcal cell wall fragments induce arthritis in rats, with the severity and duration depending on the capacity of the cells or cell fragments to resist degradation by tissue enzymes. Their phlogogenic effects are apparently related to their ability to activate the alternate complement pathway (ACP). The in vitro activation of the ACP by lysozyme-treated cells and cell walls of group A, B, and D streptococci suggests that both rat and human lysozyme can modulate this activity, i.e., increasing it, decreasing it, or doing both in that order. The effects of the lysozymes also correlated with the degree to which they can unmask the aminosugar-reducing groups detectable in a given amount of cell wall, which suggests that partial depolymerization of the cell wall is critical for ACP activation. The effects of mutanolysin and C phage lysin on ACP activation were found to be correlated with their action on streptococcal cell walls. Neuraminidase had relatively little effect on ACP activation by most streptococcal strains tested. We conclude that the participation of tissue enzymes, including but not necessarily limited to lysozyme, is an important determinant for the clinical arthritis induced by group A, B, or D streptococci. Experimental arthritis induced in rats with whole (or disrupted) streptococci may depend both on the capacities of the cell walls to activate the ACP and on the capacities of the host tissue enzymes to modulate this activation. Great severity and long durations of the disease were determined by the capacity of the enzymes to degrade cell wall antigens to a degree sufficient to ensure efficient activation of the ACP without completely degrading the material so that it no longer activates complement. In this model, the limited resistance of group B peptidoglycan to lysozyme was a critical pathogenic factor.

Published

1986