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Involvement of lectin pathway activation in the complement killing of Giardia intestinalis
Authors:Ingrid Evans-Osses  Ephraim A. Ansa-Addo  Marcel I. Ramirez
Affiliation:a Laboratório de Biologia Molecular de Parasitas e Vetores-Instituto Oswaldo Cruz-Fiocruz, Rio de Janeiro 21040-900, Brazil
b Laboratório Interdisciplinar de Pesquisas Médicas—LIP Med-Instituto Oswaldo Cruz-Fiocruz, Av. Brasil 43475, Rio de Janeiro 21040-900, Brazil
c Cellular and Molecular Immunology Research Centre, Faculty of Life Sciences, London Metropolitan University, London N7 8DB, UK
Abstract:
Giardia intestinalis (syn. G. lamblia, G. duodenalis) is a flagellated unicellular eukaryotic microorganism that commonly causes diarrheal disease throughout the world. In humans, the clinical effects of Giardia infection range from the asymptomatic carrier state to a severe malabsorption syndrome possibly due to different virulence of the Giardia strain, the number of cysts ingested, the age of the host, and the state of the host immune system at the time of infection.The question about how G. intestinalis is controlled by the organism remains unanswered. Here, we investigated the role of the complement system and in particular, the lectin pathway during Giardia infections. We present the first evidence that G. intestinalis activate the complement lectin pathway and in doing so participate in eradication of the parasite. We detected rapid binding of mannan-binding lectin, H-ficolin and L-ficolin to the surface of G. intestinalis trophozoites and normal human serum depleted of these molecules failed to kill the parasites. Our finding provides insight into the role of lectin pathway in the control of G. intestinalis and about the nature of surface components of parasite.
Keywords:Giardia intestinalis   Lectin pathway   Trophozoites   Complement-mediated killing   Intestinal disease   Mannose   GlcNAc
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