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Literature DB >> 8093695

Transfer of protective immunity in murine histoplasmosis by a CD4+ T-cell clone.

R Allendoerfer¹, D M Magee, G S Deepe, J R Graybill.

Abstract

We have reported that a murine Histoplasma capsulatum-reactive CD4+ T-cell line and clones thereof did not adoptively transfer protection against H. capsulatum infection in normal or cyclophosphamide-treated C57BL/6 mice. One explanation for the results was that the T cells failed to traffic to lymphoid organs in these animals. In this study, we have sought to determine whether one of these clones, 2.3H3, could mediate protection in nude (C57BL/10) or irradiated (5 Gy) heterozygous nude (nu/+) C57BL/6 mice. Mice were inoculated intravenously with 10(7) resting 2.3H3 cells or with an equal number of cells of the ovalbumin-reactive clone 1S6; 2 h later, the mice were challenged intranasally with 5 x 10(6) yeast cells. By day 5 of infection, lungs, livers, and spleens of nude and irradiated nu/+ mice given 2.3H3 contained significantly fewer (P < 0.05) CFU than the same organs from mice inoculated with 1S6. This effect was specific for H. capsulatum, since 2.3H3 did not reduce the number of Coccidioides immitis CFU in lungs, livers, and spleens of irradiated nu/+ mice. By day 10, the amounts of H. capsulatum CFU in lungs, livers, or spleens of nude and irradiated nu/+ mice inoculated with 2.3H3 were smaller than those in 1S6-inoculated mice, but these differences did not reach statistical significance (P > 0.05). The mortality rate of mice inoculated with 2.3H3 and that of mice inoculated with 1S6 were similar. Histopathological examination of tissues from 2.3H3- and 1S6-inoculated mice demonstrated the presence of granulomatous inflammation in organs from both groups. Tissues from 2.3H3-treated mice contained fewer yeasts per high-power field than tissues from 1S6-treated mice. Thus, irradiated or nude mice are permissive for the expression of protective immunity by a CD4+ T-cell clone. Although the protective capacity of T cells in these animals is transient, these animals will be useful for differentiating protective from nonprotective T-cell clones.

Entities: Chemical Disease Species

Mesh：

Year: 1993 PMID： 8093695 PMCID： PMC302784 DOI： 10.1128/iai.61.2.714-718.1993

Source DB: PubMed Journal: Infect Immun ISSN： 0019-9567 Impact factor: 3.441

13 in total

Review 1. Histoplasmosis and AIDS.

Authors: J R Graybill
Journal: J Infect Dis Date: 1988-09 Impact factor: 5.226

2. Role of L3T4+ T cells in host defense against Histoplasma capsulatum.

Authors: A M Gomez; W E Bullock; C L Taylor; G S Deepe
Journal: Infect Immun Date: 1988-07 Impact factor: 3.441

Review 3. Pathogenesis and clinical spectrum of histoplasmosis.

Authors: R A Goodwin; R M Des Prez
Journal: South Med J Date: 1973-01 Impact factor: 0.954

4. Risk factors for disseminated or fatal histoplasmosis. Analysis of a large urban outbreak.

Authors: L J Wheat; T G Slama; J A Norton; R B Kohler; H E Eitzen; M L French; B Sathapatayavongs
Journal: Ann Intern Med Date: 1982-02 Impact factor: 25.391

5. Protective immunity in murine histoplasmosis: functional comparison of adoptively transferred T-cell clones and splenic T cells.

Authors: G S Deepe
Journal: Infect Immun Date: 1988-09 Impact factor: 3.441

6. Inhibition of growth of Histoplasma capsulatum by lymphokine-stimulated macrophages.

Authors: B Wu-Hsieh; D H Howard
Journal: J Immunol Date: 1984-05 Impact factor: 5.422

7. Histoplasmosis in patients with the acquired immune deficiency syndrome.

Authors: W Mandell; D M Goldberg; H C Neu
Journal: Am J Med Date: 1986-12 Impact factor: 4.965

8. T-cell hybridoma-produced lymphokine that activates macrophages to suppress intracellular growth of Histoplasma capsulatum.

Authors: B Wu-Hsieh; A Zlotnik; D H Howard
Journal: Infect Immun Date: 1984-01 Impact factor: 3.441

9. Development and characterization of Histoplasma capsulatum-reactive murine T-cell lines and clones.

Authors: G S Deepe; J G Smith; G Sonnenfeld; D Denman; W E Bullock
Journal: Infect Immun Date: 1986-12 Impact factor: 3.441

10. Induction of tolerance in influenza virus-immune T lymphocyte clones with synthetic peptides of influenza hemagglutinin.

Authors: J R Lamb; B J Skidmore; N Green; J M Chiller; M Feldmann
Journal: J Exp Med Date: 1983-05-01 Impact factor: 14.307

6 in total

Transfer of protective immunity in murine histoplasmosis by a CD4+ T-cell clone.

Review 1. Histoplasmosis and AIDS.

2. Role of L3T4+ T cells in host defense against Histoplasma capsulatum.

Review 3. Pathogenesis and clinical spectrum of histoplasmosis.

4. Risk factors for disseminated or fatal histoplasmosis. Analysis of a large urban outbreak.

5. Protective immunity in murine histoplasmosis: functional comparison of adoptively transferred T-cell clones and splenic T cells.

6. Inhibition of growth of Histoplasma capsulatum by lymphokine-stimulated macrophages.

7. Histoplasmosis in patients with the acquired immune deficiency syndrome.

8. T-cell hybridoma-produced lymphokine that activates macrophages to suppress intracellular growth of Histoplasma capsulatum.

9. Development and characterization of Histoplasma capsulatum-reactive murine T-cell lines and clones.

10. Induction of tolerance in influenza virus-immune T lymphocyte clones with synthetic peptides of influenza hemagglutinin.

Review 1. Antifungal agents: chemotherapeutic targets and immunologic strategies.

2. MyD88-dependent signaling drives host survival and early cytokine production during Histoplasma capsulatum infection.

3. Intrapulmonary response to Histoplasma capsulatum in gamma interferon knockout mice.

4. Liposomal amphotericin B therapy of murine histoplasmosis.

Review 5. Cytokines and the regulation of fungus-specific CD4 T cell differentiation.

Review 6. The regulation of pulmonary immunity.