The cytolethal distending toxin of Haemophilus ducreyi aggravates dermal lesions in a rabbit model of chancroid

Haemophilus ducreyi, the etiologic agent of the sexually transmitted disease chancroid, produces a cytolethal distending toxin (HdCDT) that inhibits cultured cell proliferation, leading to cell death. A rabbit model of dermal infection was used to investigate the roles of H. ducreyi bacteria and HdC...

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Bibliographic Details
Published in:Microbes and infection 2005-05, Vol.7 (5), p.867-874
Main Authors: Wising, Catharina, Mölne, Lena, Jonsson, Ing-Marie, Ahlman, Karin, Lagergård, Teresa
Format: Article
Language:English
Subjects:
Animals
Bacterial diseases
Bacterial diseases of the genital system
Bacterial Toxins - toxicity
Bacteriology
Biological and medical sciences
Chancroid
Chancroid - pathology
Cytolethal distending toxin
Fundamental and applied biological sciences. Psychology
Haemophilus ducreyi
Haemophilus ducreyi - pathogenicity
Haemophilus Infections - pathology
Haemophilus influenzae
Human bacterial diseases
Infectious diseases
Medical sciences
Microbiology
Miscellaneous
Rabbit model
Rabbits
Skin - pathology
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Summary:Haemophilus ducreyi, the etiologic agent of the sexually transmitted disease chancroid, produces a cytolethal distending toxin (HdCDT) that inhibits cultured cell proliferation, leading to cell death. A rabbit model of dermal infection was used to investigate the roles of H. ducreyi bacteria and HdCDT in the development, clinical appearance, and persistence of infection. A non-toxin producing H. ducreyi strain, and for comparison purposes a non-capsulated Haemophilus influenzae strain, were inoculated intradermally, with and without co-administration of purified HdCDT. Co-administration of HdCDT resulted in significant aggravation of H. ducreyi-induced inflammatory lesions, and development of ulcers in rabbit skin. Less pronounced inflammatory lesions and lack of epithelial eruption were observed after inoculation with H. influenzae. Histopathological sections of the H. ducreyi-induced lesions, in both the presence and absence of HdCDT, showed dense infiltrates of the same type inflammatory cells, with the exception of a prominent endothelial cell proliferation noted in sections from lesions caused by H. ducreyi and toxin. Signs of chronic inflammation with involvement of T cells, macrophages, eosinophils, and granuloma formation were observed after H. ducreyi inoculation both with and without toxin. In conclusion, H. ducreyi causes a pronounced, chronic inflammation with involvement of T cells and macrophages, and in combination with HdCDT production of ulcers in the rabbit model. These pathogenic mechanisms may promote the development and persistence of chancroid ulcers.
ISSN:1286-4579
1769-714X
DOI:10.1016/j.micinf.2005.02.009