Rapid Clonal Expansion and Prolonged Maintenance of Memory CD8+ T Cells of the Effector (CD44highCD62Llow) and Central (CD44highCD62Lhigh) Phenotype by an Archaeosome Adjuvant Independent of TLR2

Krishnan, Lakshmi; Gurnani, Komal; Dicaire, Chantal J.; Faassen, Henk van; Zafer, Ahmed; Kirschning, Carsten J.; Sad, Subash; Sprott, G. Dennis

doi:10.4049/jimmunol.178.4.2396

Cited by 44 publications

(40 citation statements)

References 57 publications

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“…* , compared to 9241(pYA3634)-immunized mice, the P value was Ͻ0.05; ** , compared to 9241(pYA3634)-immunized mice, the P value was Ͻ0.01. (25). Therefore, we evaluated the effect of ⌬sopB on the stimulation of a memory T-cell response.…”

Section: Resultsmentioning

confidence: 99%

AsopBDeletion Mutation Enhances the Immunogenicity and Protective Efficacy of a Heterologous Antigen Delivered by Live AttenuatedSalmonella entericaVaccines

Wang

Wei

et al. 2008

Infect Immun

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SopB is a virulence factor of Salmonella encoded by SPI-5. Salmonella sopB deletion mutants are impaired in their ability to cause local inflammatory responses and fluid secretion into the intestinal lumen and also can enhance the immunogenicity of a vectored antigen. In this study, we evaluated the effects on immunogenicity and the efficacy of a sopB deletion mutation on two Salmonella enterica serovar Typhimurium vaccine strains with different attenuating mutations expressing a highly antigenic ␣-helical region of the Streptococcus pneumoniae surface protein PspA from an Asd ؉ -balanced lethal plasmid. After oral administration to mice, the two pairs of strains induced high levels of serum antibodies specific for PspA as well as to Salmonella antigens. The levels of antigen-specific serum immunoglobulin G (IgG) and mucosal IgA were higher in mice immunized with sopB mutants. Enzyme-linked immunospot assay results indicated that the spleen cells from mice immunized with a sopB mutant showed higher interleukin-4 and gamma interferon secretion levels than did the mice immunized with the isogenic sopB ؉ strain. The sopB mutants also induced higher numbers of CD4 ؉ CD44 hi CD62L hi and CD8 ؉ CD44 hi CD62L hi central memory T cells. Eight weeks after primary oral immunization, mice were challenged with 100 50% lethal doses of virulent S. pneumoniae WU2. Immunization with either of the sopB mutant strains led to increased levels of protection compared to that with the isogenic sopB ؉ parent. Together, these results demonstrate that the deletion of sopB leads to an overall enhancement of the immunogenicity and efficacy of recombinant attenuated Salmonella vaccine strains.

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Section: Resultsmentioning

confidence: 99%

AsopBDeletion Mutation Enhances the Immunogenicity and Protective Efficacy of a Heterologous Antigen Delivered by Live AttenuatedSalmonella entericaVaccines

Wang

Wei

et al. 2008

Infect Immun

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“…Naive T cells express CD62L (L-selectin), which is known to be a homing receptor, and shed this molecule to migrate from lymphoid organs to inflammatory sites after activation [18]. CD44 appears to be the most reliable marker that is expressed at high levels in all memory T cells of mice, irrespective of their activation status [19]. CD8 1 T cells can be classified into three groups according to their expression patterns of CD62L and CD44: CD62L hi CD44 lo , CD62L hi CD44 hi and CD62L lo CD44 hi patterns represent naive, central memory, and effector memory phenotypes, respectively [19].…”

Section: Immunophenotype Characterization Of Cd8 1 T Cells In Immune mentioning

confidence: 99%

“…CD44 appears to be the most reliable marker that is expressed at high levels in all memory T cells of mice, irrespective of their activation status [19]. CD8 1 T cells can be classified into three groups according to their expression patterns of CD62L and CD44: CD62L hi CD44 lo , CD62L hi CD44 hi and CD62L lo CD44 hi patterns represent naive, central memory, and effector memory phenotypes, respectively [19]. Spleen cells from recipient mice transferred with the indicated cells were analyzed 7 days after infection with PyL ( Fig.…”

Section: Immunophenotype Characterization Of Cd8 1 T Cells In Immune mentioning

confidence: 99%

Involvement of CD8⁺ T cells in protective immunity against murine blood‐stage infection with Plasmodium yoelii 17XL strain

et al. 2010

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When developing malaria vaccines, the most crucial step is to elucidate the mechanisms involved in protective immunity against the parasites. We found that CD8+ T cells contribute to protective immunity against infection with blood‐stage parasites of Plasmodium yoelii. Infection of C57BL/6 mice with P. yoelii 17XL was lethal, while all mice infected with a low‐virulence strain of the parasite 17XNL acquired complete resistance against re‐infection with P. yoelii 17XL. However, the host mice transferred with CD8+ T cells from mice primed only with P. yoelii 17XNL failed to acquire protective immunity. On the other hand, the irradiated host mice were completely resistant to P. yoelii 17XL infection, showing no grade of parasitemia when adoptively transferred with CD8+ T cells from immune mice that survived infection with both P. yoelii XNL and, subsequently, P. yoelii 17XL. These protective CD8+ T cells from immune WT mice had the potential to generate IFN‐γ, perforin (PFN) and granzyme B. When mice deficient in IFN‐γ were used as donor mice for CD8+ T cells, protective immunity in the host mice was fully abrogated, and the immunity was profoundly attenuated in PFN‐deficient mice. Thus, CD8+ T cells producing IFN‐γ and PFN appear to be involved in protective immunity against infection with blood‐stage malaria.

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“…Although the repertoire of T cell activation markers is rapidly expanding, 30 the relative levels of CD44 and CD62L are frequently used to distinguish naïve (CD44 lo CD62L hi ) from effector (CD44 hi CD62L lo ) T cells. [31][32][33][34][35][36][37] In the M. leprae-infected FPs, the majority of CD4 ϩ and CD8 ϩ cells were of the effector phenotype, expressing CD44 hi CD62L lo (87.77 Ϯ 1.62% and 82.76 Ϯ 1.93, respectively). We also attempted to evaluate the cellular composition of the cLT␣ Ϫ/Ϫ FPs by flow cytometry; however, we were unsuccessful as these preparations lacked sufficient numbers of leukocytes for a reliable assessment.…”

Section: Immune Cell Composition Of the M Leprae-infected Fpsmentioning

confidence: 99%

Lymphotoxin-α and TNF Have Essential but Independent Roles in the Evolution of the Granulomatous Response in Experimental Leprosy

Hagge

Saunders

Ebenezer³

et al. 2009

The American Journal of Pathology

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Recent studies identified an association between genetic variants in the lymphotoxin-␣ (LT␣) gene and leprosy.To study the influence of LT␣ on the control of experimental leprosy, both low-and high-dose Mycobacterium leprae foot pad (FP) infections were evaluated in LT␣-deficient chimeric (cLT␣ On infection with many intracellular organisms, especially mycobacterial pathogens, a granulomatous response ensues. This complex process involves the participation of cell-mediated immunity (CMI), activation of endothelial cells, enhancement of adhesion molecule expression, management of macrophage and lymphocyte infiltration, and induction of the microbiostatic and microbicidal effects of macrophages.1 In addition, extensive intercellular communication, chiefly through cytokine and chemokine signals, is required to orchestrate this cellular accumulation and results in a three-dimensional structure that limits or prevents dissemination of the pathogen and is largely protective.The contributions of both soluble and membranebound tumor necrosis factor (TNF) to granuloma development have been established.2-5 Lymphotoxin (LT)-␣ is also a member of the TNF superfamily, but as compared with TNF, much less is known about its function. LT␣ is required for the development of secondary lymphoid tissue 6 through its association with LT␤, to form heterotrimeric LT␣ 1 ␤ 2 and LT␣ 2 ␤ 1 , which enable interaction between lymphocytes and surrounding fibroblasts, and epithelial and myeloid cells that express the LT␤ receptor. Current evidence also suggests that LT␣ plays a regulatory role in CMI 7 and serves as an initiating stimuSupported by National Institutes of Health (NIH) grant AI-50027 (L. Adams) and the NHMRC of Australia (B. Saunders and W. Britton).

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Rapid Clonal Expansion and Prolonged Maintenance of Memory CD8+ T Cells of the Effector (CD44highCD62Llow) and Central (CD44highCD62Lhigh) Phenotype by an Archaeosome Adjuvant Independent of TLR2

Cited by 44 publications

References 57 publications

AsopBDeletion Mutation Enhances the Immunogenicity and Protective Efficacy of a Heterologous Antigen Delivered by Live AttenuatedSalmonella entericaVaccines

AsopBDeletion Mutation Enhances the Immunogenicity and Protective Efficacy of a Heterologous Antigen Delivered by Live AttenuatedSalmonella entericaVaccines

Involvement of CD8⁺ T cells in protective immunity against murine blood‐stage infection with Plasmodium yoelii 17XL strain

Lymphotoxin-α and TNF Have Essential but Independent Roles in the Evolution of the Granulomatous Response in Experimental Leprosy

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Rapid Clonal Expansion and Prolonged Maintenance of Memory CD8+ T Cells of the Effector (CD44highCD62Llow) and Central (CD44highCD62Lhigh) Phenotype by an Archaeosome Adjuvant Independent of TLR2

Cited by 44 publications

References 57 publications

AsopBDeletion Mutation Enhances the Immunogenicity and Protective Efficacy of a Heterologous Antigen Delivered by Live AttenuatedSalmonella entericaVaccines

AsopBDeletion Mutation Enhances the Immunogenicity and Protective Efficacy of a Heterologous Antigen Delivered by Live AttenuatedSalmonella entericaVaccines

Involvement of CD8+ T cells in protective immunity against murine blood‐stage infection with Plasmodium yoelii 17XL strain

Lymphotoxin-α and TNF Have Essential but Independent Roles in the Evolution of the Granulomatous Response in Experimental Leprosy

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Involvement of CD8⁺ T cells in protective immunity against murine blood‐stage infection with Plasmodium yoelii 17XL strain