Gene/Protein Disease Symptom Drug Enzyme Compound
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Query: UMLS:C0017536 (giardiasis)
 1,714 document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)

In vivo, epithelial cells which line the intestine are intimately associated with lymphocytes, termed intraepithelial lymphocytes. Previous studies have demonstrated that intraepithelial lymphocytes are present in the uninflamed mucosa, and become especially prominent in various human enteropathies including coeliac disease, tropical sprue, dermatitis herpetiformis, and giardiasis. Using the intestinal crypt cell line T84, and a previously well-defined human mucosa-derived lymphocyte (MDL) line with phenotypic features similar to (but not specific for) intraepithelial lymphocytes, we describe a co-culture model to study the functional sequellae of MDL-T84 cell interactions in vitro. A co-culture method was defined which permitted reconstitution of the paracellular spaces of physiologically confluent epithelial monolayers with MDL. Such co-cultures thus mimicked the correct geometry of intraepithelial lymphocytes-epithelial cell interactions. The presence of physiologically positioned MDL brought about specific and dramatic effects on intestinal epithelial monolayer function. In a dose-dependent fashion, the presence of MDL significantly attenuated barrier function (expressed as a decrease in monolayer resistance), decreased epithelial electrogenic Cl- secretion, and modulated epithelial-neutrophil interactions. Such effects were not reproduced in monolayers similarly reconstituted with inert polystyrene beads equivalent in size to MDL. These MDL-elicited effects on epithelial function specifically required direct MDL apposition to the epithelial basolateral membrane. Furthermore, this specific form of MDL-epithelial basolateral contact released soluble factors which were able to confer the MDL-reconstituted phenotype on virgin epithelial monolayers in the absence of MDL. We have previously shown that many aspects of the MDL converted epithelial phenotype described here can be induced by IFN-gamma. While IFN-gamma, a cytokine produced by many lymphocytes including intraepithelial lymphocytes, was detectable in conditioned supernatants from co-cultures, it existed at concentrations insufficient to fully explain the physiologic effects observed here.
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PMID:Reconstitution of cultured intestinal epithelial monolayers with a mucosal-derived T lymphocyte cell line. Modulation of epithelial phenotype dependent on lymphocyte-basolateral membrane apposition. 804 Mar 34

This work studied the effect of sub-chronic DDT exposure on the course of experimental giardiasis and efficacy of its treatment. A total of 160 mice were divided into six groups: G1: 30 mice received DDT and infected with Giardia lamblia. G2: 30 mice received DDT, infected and treated with tinidazole (TNZ). G3: 30 mice infected with Giardia. G4: 30 mice infected and treated with TNZ. G5: 30 mice received DDT only. G6: 10 mice served as normal control. Mice were sacrificed at 7, 14, 21 & 28 days P.I. All groups were subjected to cyst count/2 hours collected stool, trophozoite count in intestine, histopathological examination of small intestinal section and avidin biotin peroxidase technique for local IgA staining. Also, IFN-gamma was measured in sera. DDT caused early shedding of many cysts and increase in trophozoite counts for a long time, decreased intra epithelial lymphocytes, low levels of IgA & IFN-gamma and severe histopathological changes in intestinal sections in G1 as compared to G3. Also, DDT reduced the efficacy of TNZ treatment in G2 as compared to G4. The results strongly support the immunomodulating effect of DDT on experimental giardiasis that might be responsible for persistence of infection, resistance to treatment and re-infection in DDT exposed persons.
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PMID:Effect of organochlorine (DDT) exposure on experimental giardiasis. 1914 33