Sequestration of host-CD59 as potential immune evasion strategy of Trichomonas vaginalis

Sequestration of host-CD59 as potential immune evasion strategy of Trichomonas vaginalis

•No sequence homology in Trichomonas vaginalis genome with CD59 human gene.•IFI detection of CD59 on T. vaginalis surface of flagellates recovered from mice.•No CD59 on T. vaginalis from batch cultures, only those co-cultivated with mice RBC.•T. vaginalis cultures supplemented with RBC were more res...

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Veröffentlicht in:Acta tropica 2015-09, Vol.149, p.1-7
Hauptverfasser: Ibáñez-Escribano, Alexandra, Nogal-Ruiz, Juan José, Pérez-Serrano, Jorge, Gómez-Barrio, Alicia, Escario, J. Antonio, Alderete, J.F.
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Antibodies, Monoclonal
Ascites
CD59
CD59 Antigens - metabolism
Complement
Complement System Proteins - immunology
Erythrocytes
Erythrocytes - immunology
Fluorescence
Fluorescent Antibody Technique
Human sera
Humans
Immune Evasion
Mice
Trichomonas vaginalis
Trichomonas vaginalis - genetics
Trichomonas vaginalis - metabolism
Trichomonas vaginalis - pathogenicity
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Zusammenfassung:•No sequence homology in Trichomonas vaginalis genome with CD59 human gene.•IFI detection of CD59 on T. vaginalis surface of flagellates recovered from mice.•No CD59 on T. vaginalis from batch cultures, only those co-cultivated with mice RBC.•T. vaginalis cultures supplemented with RBC were more resistant against human serum.•Results suggest host-CD59 acquisition as an additional immune evasion strategy. Trichomonas vaginalis is known to evade complement-mediated lysis. Because the genome of T. vaginalis does not possess DNA sequence with homology to human protectin (CD59), a complement lysis restricting factor, we tested the hypothesis that host CD59 acquisition by T. vaginalis organisms mediates resistance to complement killing. This hypothesis was based on the fact that trichomonads are known to associate with host proteins. No CD59 was detected on the surface of T. vaginalis grown in serum-based medium using as probe anti-CD59 monoclonal antibody (MAb). We, therefore, infected mice intraperitoneally with live T. vaginalis, and trichomonads harvested from ascites were tested for binding of CD59. Immunofluorescence showed that parasites had surface CD59. Furthermore, as mouse erythrocytes (RBCs) possess membrane-associated CD59, and trichomonads use RBCs as a nutrient source, organisms were co-cultured with murine RBCs for one week. Parasites were shown to have detectable surface CD59. Importantly, live T. vaginalis with bound CD59 were compared with batch-grown parasites without surface-associated CD59 for sensitivity to complement in human serum. Trichomonads without surface-bound CD59 had a higher level of killing by complement than did parasites with surface CD59. These data show that host CD59 acquired onto the surface by live T. vaginalis may be an alternative mechanism for complement evasion. We describe a novel strategy by T. vaginalis consistent with host protein procurement by this parasite to evade the lytic action of complement.
ISSN:0001-706X
1873-6254
DOI:10.1016/j.actatropica.2015.05.003