Bedoukian   RussellIPM   RussellIPM   Piezoelectric Micro-Sprayer


Home
Animal Taxa
Plant Taxa
Semiochemicals
Floral Compounds
Semiochemical Detail
Semiochemicals & Taxa
Synthesis
Control
Invasive spp.
References

Abstract

Guide

Alphascents
Pherobio
InsectScience
E-Econex
Counterpart-Semiochemicals
Print
Email to a Friend
Kindly Donate for The Pherobase

« Previous AbstractAggregation and binding substances enhance pathogenicity in a rabbit model of Enterococcus faecalis endocarditis    Next Abstract"Aggregation of the Whi3 protein, not loss of heterochromatin, causes sterility in old yeast cells" »

Infect Immun


Title:Aggregation and binding substances enhance pathogenicity in rabbit models of Enterococcus faecalis endocarditis
Author(s):Schlievert PM; Gahr PJ; Assimacopoulos AP; Dinges MM; Stoehr JA; Harmala JW; Hirt H; Dunny GM;
Address:"Department of Microbiology, University of Minnesota Medical School, Minneapolis 55455-0312, USA. pats@lenti.med.umn.edu"
Journal Title:Infect Immun
Year:1998
Volume:66
Issue:1
Page Number:218 - 223
DOI: 10.1128/IAI.66.1.218-223.1998
ISSN/ISBN:0019-9567 (Print) 1098-5522 (Electronic) 0019-9567 (Linking)
Abstract:"We investigated the importance of enterococcal aggregation substance (AS) and enterococcal binding substance (EBS) in rabbit models of Enterococcus faecalis cardiac infections. First, American Dutch belted rabbits were injected intraventricularly with 10(8) CFU and observed for 2 days. No clinical signs of illness developed in animals given AS- EBS- organisms, and all survived. All rabbits given AS- EBS+ organisms developed signs of illness, including significant pericardial inflammation, but only one of six died. All animals given AS+ EBS- organisms developed signs of illness, including pericardial inflammation, and survived. All rabbits given AS+ EBS+ organisms developed signs of illness and died. None of the rabbits receiving AS+ EBS+ organisms showed gross pericardial inflammation. The lethality and lack of inflammation are consistent with the presence of a superantigen. Rabbit and human lymphocytes were highly stimulated in vitro by cell extracts, but not cell-free culture fluids, of AS+ EBS+ organisms. In contrast, cell extracts from AS- EBS- organisms weakly stimulated lymphocyte proliferation. Culture fluids from human lymphocytes stimulated with AS+/EBS+ enterococci contained high levels of gamma interferon and tumor necrosis factor alpha (TNF-alpha) and TNF-beta, which is consistent with functional stimulation of T-lymphocyte proliferation and macrophage activation. Subsequent experiments examined the abilities of the same strains to cause endocarditis in a catheterization model. New Zealand White rabbits underwent transaortic catheterization for 2 h, at which time catheters were removed and animals were injected with 2 x 10(9) CFU of test organisms. None of the animals given AS- EBS- organisms developed vegetations or showed autopsy evidence of tissue damage. Rabbits given AS- EBS+ or AS+ EBS- organisms developed small vegetations and had splenomegaly at autopsy. All rabbits given AS+ EBS+ organisms developed large vegetations and had splenomegaly and lung congestion at autopsy. Similar experiments that left catheters in place for 3 days revealed that all rabbits given AS- EBS- or AS+ EBS+ organisms developed vegetations, but animals given AS+ EBS+ organisms had larger vegetations and autopsy evidence of lung congestion. These experiments provide direct evidence that these two cell wall components play an important role in the pathogenesis of endocarditis as well as in conjugative plasmid transfer"
Keywords:"Adhesins, Bacterial/*genetics/*metabolism/physiology Animals Bacterial Adhesion Bacterial Proteins/genetics Catheterization/adverse effects Cell Division Cell Extracts/immunology/pharmacology Cells, Cultured Culture Media, Conditioned/pharmacology Endocar;"
Notes:"MedlineSchlievert, P M Gahr, P J Assimacopoulos, A P Dinges, M M Stoehr, J A Harmala, J W Hirt, H Dunny, G M eng T32 HD007381/HD/NICHD NIH HHS/ HL51987/HL/NHLBI NIH HHS/ R01 HL051987/HL/NHLBI NIH HHS/ 2-T32-HD-07381/HD/NICHD NIH HHS/ 2-T32-AI-07421/AI/NIAID NIH HHS/ T32 AI007421/AI/NIAID NIH HHS/ Research Support, U.S. Gov't, P.H.S. 1998/01/10 Infect Immun. 1998 Jan; 66(1):218-23. doi: 10.1128/IAI.66.1.218-223.1998"

 
Back to top
 
Citation: El-Sayed AM 2024. The Pherobase: Database of Pheromones and Semiochemicals. <http://www.pherobase.com>.
© 2003-2024 The Pherobase - Extensive Database of Pheromones and Semiochemicals. Ashraf M. El-Sayed.
Page created on 28-12-2024