ABSTRACT
MF6p/FhHDM-1 is a small cationic heme-binding protein which is recognized by the monoclonal antibody (mAb) MF6, and abundantly present in parenchymal cells and secreted antigens of Fasciola hepatica. Orthologs of this protein (MF6p/HDMs) also exist in other causal agents of important foodborne trematodiasis, such as Clonorchis sinensis, Opisthorchis viverrini and Paragonimus westermani. Considering that MF6p/FhHDM-1 is relevant for heme homeostasis in Fasciola and was reported to have immunomodulatory properties, this protein is expected to be a useful target for vaccination. Thus, in this study we mapped the epitope recognized by mAb MF6 and evaluated its antigenicity in sheep. The sequence of the MF6p/FhHDM-1 ortholog from F. gigantica (MF6p/FgHDM-1) was also reported. By means of ELISA inhibitions with overlapping synthetic peptides, we determined that the epitope recognized by mAb MF6 is located within the C-terminal moiety of MF6p/FhHDM-1, which is the most conserved region of MF6p/HDMs. By immunoblotting analysis of parasite extracts and ELISA inhibitions with synthetic peptides we also determined that mAb MF6 reacted with the same intensity with F. hepatica and F. gigantica, and in decreasing order of intensity with C. sinensis, O.viverrini and P. westermani orthologs. On the contrary, mAb MF6 showed no reactivity against Dicrocoelium dendriticum and Schistosoma mansoni. The study of the recognition of peptides covering different regions of MF6p/FhHDM-1 by sera from immunized sheep revealed that the C-terminal moiety is the most antigenic, thus being of potential interest for vaccination. We also demonstrated that the production of antibodies to MF6p/FhHDM-1 in sheep infected by F. hepatica occurs relatively early and follows the same pattern as those produced against L-cathepsins.
Subject(s)
Carrier Proteins/chemistry , Fasciola hepatica/immunology , Fascioliasis/immunology , Heme/immunology , Hemeproteins/chemistry , Animals , Antibodies, Helminth/chemistry , Antibodies, Helminth/immunology , Antibodies, Monoclonal/immunology , Antigens, Helminth/chemistry , Antigens, Helminth/immunology , Carrier Proteins/immunology , Dendrites/immunology , Dendrites/parasitology , Enzyme-Linked Immunosorbent Assay , Epitope Mapping , Epitopes/immunology , Fasciola hepatica/pathogenicity , Fascioliasis/parasitology , Heme/chemistry , Heme/metabolism , Heme-Binding Proteins , Hemeproteins/immunology , Protein Conformation , Sheep/immunology , Sheep/parasitology , VaccinationABSTRACT
A comparison has been made between the chaetotaxy of the gyrodactylid monogeneans Macrogyrodactylus clarii Gussev, 1961 and M. congolensis (Prudhoe, 1957) Yamaguti, 1963 from the gills and skin, respectively, of the catfish Clarias gariepinus (Burchell) from the river Nile in Egypt. Bilaterally arranged argentophilic structures on the surface of these parasites are presumed to be sensilla and are more abundant in M. clarii than in M. congolensis especially on the ventral surface (124 vs. 66). In both species these sensilla are concentrated on the head lobes and in the pharyngeal region, but there are features of the sensilla patterns that can be used to distinguish the two species. Comparison is made with sensilla patterns of other gyrodactylids. A system of cells and dendritic processes, most probably part of the nervous system, also has an affinity for silver in the two species. There are no previous records of extensive argentophilic elements in the nervous systems of monogeneans.
Subject(s)
Catfishes/parasitology , Gills/parasitology , Skin/parasitology , Trematoda/classification , Trematoda/ultrastructure , Animals , Dendrites/parasitology , Dendrites/ultrastructure , Egypt , Nervous System/ultrastructure , Photomicrography , Silver Staining/methods , Species SpecificityABSTRACT
The question we attempted to address in this chapter is: Do brief but recurrent seizures in early life alter the ontogeny of hippocampal networks in ways that produce epileptic circuits? Results from the tetanus toxin model suggest that this is likely the case. Following seizures in Postnatal Weeks 2 and 3, most adult rats have a focal epilepsy that arises from hippocampus. Recordings from hippocampal slices support this conclusion since they demonstrated the occurrence of spontaneous network discharges in normal artificial cerebrospinal fluid. Moreover, when GABA-A receptor-mediated synaptic transmission was suppressed, slices from adult epileptic rats produced prolonged electrographic seizures which are never observed in control rats. This suggests that hyperexcitable recurrent excitatory networks contribute to hippocampal seizures in this model. In light of this, anatomical results from biocytin-filled neurons were surprising. Results suggest that recurrent axon arbors neither sprout additional branches as a result of seizure activity nor maintain their exuberant branching patterns of early life. Thus, excessive connectivity cannot explain seizure generation. Axon arbors either remodel in normal ways or prune additional collaterals as a result of ongoing epileptiform discharging. At the same time that axon arbors remodel, the dendrites of these cells have decreased dendritic spine density, suggesting a partial deafferentation. While a complete understanding of the origins of spine loss requires further investigation, we hypothesize that this loss is a product of a partial deafferentation that occurs due to excessive and abnormal selection of synaptic connections. Network-induced heterosynaptic LTD of noncoincidentally active afferants may be one mechanism that leads to a loss of synapses. Moreover, competition among and selection between individual recurrent excitatory synapses may contribute to spine loss as well. The "winners" of this competition, the most potent and effective early-formed recurrent excitatory synapses, are likely key contributors to seizure generation in this model and possibly in humans with early-onset temporal lobe epilepsy.
