Assessment in vitro of immunity against Toxoplasma gondii.

Jones, Thomas C.; Len, L; Hirsch, James G.

doi:10.1084/jem.141.2.466

Cited by 134 publications

(79 citation statements)

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“…The macrophage as an element in host-parasite interactions is by no means unique to encephalitozoonosis but is a common participant in other intracellular protozoal infections, especially toxoplasmosis. 16 In both toxoplasmosis and encephalitozoonosis, the quiescent macrophage does not kill the p a r a~i t e~~,~~ but requires activation through lymphokine p r o d u~t s~l ,~~ or parasite opsonization by antibody. 1,35, 48 Although not addressed within these experiments, sensitized canine lymphocytes most likely do produce soluble products when exposed to E. cuniculi antigens.…”

Section: Discussionmentioning

confidence: 99%

Experimental Encephalitozoonosis in Neonatal Dogs

Szabo

Shadduck

1987

Vet Pathol

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Abstract. The in vivo infection of neonatal dogs by the microsporidian protozoan parasite, Encephalitozoon cuniculi, was studied. Microscopic examination of tissues from infected animals showed granulomatous nephritis, meningoencephalitis, hepatitis, and pneumonitis. A large component of the inflammatory infiltrate consisted of plasma cells and lymphocytes. In addition, hyperplasia of B-lymphocyte-dependent regions of lymph nodes and erythrophagocytosis were consistently seen in infected dogs. Infected dogs developed lymphocytosis, hypergammaglobulinemia, anti-encephalitozoon antibodies, and an antigen-specific blastogenic response to E. cuniculi spores. Lymphocyte blastogenic responses to the lectin phytohemagglutinin A (PHA) were depressed compared to controls. Dogs dying during the 2-month experimental trial were bacteremic. The findings of these experiments suggest that postnatal infection results in a demonstrable although seemingly ineffective immune and inflammatory response without detectable clinical disease.

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Section: Discussionmentioning

confidence: 99%

Experimental Encephalitozoonosis in Neonatal Dogs

Szabo

Shadduck

1987

Vet Pathol

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“…Soluble antigen was prepared from the RH strain of T. gondii as previously described [10]. All five subjects studied were pretested in an eight-day lymphocyte transformation assay with the antigen to determine the optimal dose for maximal proliferation.…”

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confidence: 99%

Association of Symptomatic Human Infection with Toxoplasma gondii with Imbalance of Monocytes and Antigen-Specific T Cell Subsets

Sklenar¹,

Jones²,

Alkan³

et al. 1986

Journal of Infectious Diseases

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During. recent symptomatic toxoplasmosis, alterations in quantity and function of mononuclear cellsin peripheral blood were observed. Flow cytofluorometric analysis and differential leukocyte counts revealed increasedabsolute numbers of T8 + cells, Leu 7 + (natural killer/killer) cells, and monocytes. T4+ cells and HLA-DR+ cells were not significantly changed. T4/T8 cell ratios were reversed in symptomatic toxoplasmosis (0.7 ± 0.3) and normal in chronic infection (1.7 ± 0.5). Toxoplasma antigen induced higher numbers of T8 -+-aridTQl + cells in four T cell lines from two individuals with symptomatic infection than in five T cell lines from three individuals with asymptomatic infection. Eight cloned T cell lines produced y interferon in an antigen-specific fashion and in higher amounts when they originated from an asymptomatic subject than from a symptomatic subject. These results indicate that marked alterations in properties of immunoregulatory cells are characteristic of recent symptomatic toxoplasmosis. The transient immune dysfunction may be a major part of the observed disease and/or a feature of successful parasitism.Infection with the coccidian protozoan Toxoplasma gondii causes no illness in most individuals. In about one of five infected individuals, various degrees of fatigue, malaise, fever, and lymph node enlargement are recorded [1]. These subjects recover without residual signs of disease; this distinguishes them from those with documented immune deficiency, in whom toxoplasmosis is often severe and even fatal [2]. It has also been noted that evidence of cellular immune response to toxoplasma antigens is delayed in appearance in some patients, compared with the kinetics of response to other antigens [1,3,4]. In an effort to understand better immune responses during acute symptomatic infection, we examined total T cell subsets and toxoplasma antigen-induced T cell subsets during toxoplasmosis. Informed consent was obtained from all human subjects studied.This work was supported by grant 3.016.-0.84 from the Swiss National Science Foundation.We thank MartinWesp (Ciba-Geigy, Basel, Switzerland) for help with the Cytofluorograph analyses and Danielle Rieder for technical assistance.Please address requests for reprints to Dr. Ivo Sklenar, Institute for Microbiology and Hygiene, University of Basel, Petersplatz 10, CH-4003 Basel, Switzerland. Subjects and MethodsSubjects. A total of 22 individuals was studied.T cell surface markers of peripheral blood lymphocytes (PBLs) were studied in 19 individuals with use of monoclonal antibodies and a Cytofluorographs' (Ortho Instruments, West Wood, Mass). According to the history of infection by T. gondii, three groups of subjects were defined. Six Iloninfected individuals (mean ± SD age, 29 ± 11 years) were compared with five chronically infected individuals (mean ± SD age, 33 ± 7 years) and eight patients with recent symptomatic toxoplasmosis (mean ± SD age, 26 ± 6 years).The noninfected individuals were negative for IgG antibody to Toxoplasma by the immunofluore...

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“…At present, the mechanism whereby the macrophages incubated with Toxo-GIF inhibit multiplication of Toxoplasma is unknown. Several workers reported that Toxoplasma-immune macrophages showed a prolonged lag phase and increased generation time compared to nonimmune macrophages (2,11,23). Our unpublished observations indicated that by incubation with Toxo-GIF, glycogen-induced nonimmune macrophages showed prolonged lag phases (18-22 hr) compared to those of control macrophages (10-1 1 hr).…”

Section: Discussionmentioning

confidence: 99%

“…Recent studies with Toxoplasma infection have shown that cell-mediated immunity plays a major role in resistance to infection with this obligate intracellular pathogen (2,5,8,11,18). Lymphocytes from immunized donors produce in response to antigenic stimulation a variety of biologically active substances which have been collectively termed "lymphokines".…”

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confidence: 99%