Your search keyword '"Oftung Fredrik"' showing total 4 results

1. FLU-v, a Broad-Spectrum Influenza Vaccine, Induces Cross-Reactive Cellular Immune Responses in Humans Measured by Dual IFN-γ and Granzyme B ELISpot Assay.

Author

Oftung, Fredrik, Næss, Lisbeth M., Laake, Ida, Stoloff, Gregory, and Pleguezuelos, Olga

Subjects

INFLUENZA vaccines, GRANZYMES, IMMUNE response, B cells, CELL physiology, VIRAL shedding, INFLUENZA, HUMORAL immunity

Abstract

Previous reports demonstrated that FLU-v, a peptide-based broad-spectrum influenza vaccine candidate, induced antibody and cellular immune responses in humans. Here, we evaluate cellular effector functions and cross-reactivity. PBMC sampled pre- (day 0) and post-vaccination (days 42 and 180) from vaccine (n = 58) and placebo (n = 27) recipients were tested in vitro for responses to FLU-v and inactivated influenza strains (A/H3N2, A/H1N1, A/H5N1, A/H7N9, B/Yamagata) using IFN-γ and granzyme B ELISpot. FLU-v induced a significant increase in the number of IFN-γ- and granzyme-B-secreting cells responding to the vaccine antigens from pre-vaccination (medians: 5 SFU/106 cells for both markers) to day 42 (125 and 40 SFU/106 cells, p < 0.0001 for both) and day 180 (75 and 20 SFU/106 cells, p < 0.0001 and p = 0.0047). The fold increase from pre-vaccination to day 42 for IFN-γ-, granzyme-B-, and double-positive-secreting cells responding to FLU-v was significantly elevated compared to placebo (medians: 16.3-fold vs. 1.0-fold, p < 0.0001; 3.5-fold vs. 1.0-fold, p < 0.0001; 3.0-fold vs. 1.0-fold, p = 0.0012, respectively). Stimulation of PBMC with inactivated influenza strains showed significantly higher fold increases from pre-vaccination to day 42 in the vaccine group compared to placebo for IFN-γ-secreting cells reacting to H1N1 (medians: 2.3-fold vs. 0.8-fold, p = 0.0083), H3N2 (1.7-fold vs. 0.8-fold, p = 0.0178), and H5N1 (1.7-fold vs. 1.0-fold, p = 0.0441); for granzyme B secreting cells reacting to H1N1 (3.5-fold vs. 1.0-fold, p = 0.0075); and for double positive cells reacting to H1N1 (2.9-fold vs. 1.0-fold, p = 0.0219), H3N2 (1.7-fold vs. 0.9-fold, p = 0.0136), and the B strain (2.0-fold vs. 0.8-fold, p = 0.0227). The correlation observed between number of cells secreting IFN-γ or granzyme B in response to FLU-v and to the influenza strains supported vaccine-induced cross-reactivity. In conclusion, adjuvanted FLU-v vaccination induced cross-reactive cellular responses with cytotoxic capacity, further supporting the development of FLU-v as a broad-spectrum influenza vaccine. [ABSTRACT FROM AUTHOR]

Published

2022

2. Immune Responses in Acute and Convalescent Patients with Mild, Moderate and Severe Disease during the 2009 Influenza Pandemic in Norway.

Author

Mohn, Kristin G.-I., Cox, Rebecca Jane, Tunheim, Gro, Berdal, Jan Erik, Hauge, Anna Germundsson, Jul-Larsen, Åsne, null, null, Peters, Bjoern, Oftung, Fredrik, Jonassen, Christine Monceyron, and Mjaaland, Siri

Subjects

IMMUNE response, INFLUENZA, TUMOR necrosis factors, T cells, HOSPITAL admission & discharge, CD8 antigen, PATIENTS, PHYSIOLOGY

Abstract

Increased understanding of immune responses influencing clinical severity during pandemic influenza infection is important for improved treatment and vaccine development. In this study we recruited 46 adult patients during the 2009 influenza pandemic and characterized humoral and cellular immune responses. Those included were either acute hospitalized or convalescent patients with different disease severities (mild, moderate or severe). In general, protective antibody responses increased with enhanced disease severity. In the acute patients, we found higher levels of TNF-α single-producing CD4+T-cells in the severely ill as compared to patients with moderate disease. Stimulation of peripheral blood mononuclear cells (PBMC) from a subset of acute patients with peptide T-cell epitopes showed significantly lower frequencies of influenza specific CD8+ compared with CD4+ IFN-γ T-cells in acute patients. Both T-cell subsets were predominantly directed against the envelope antigens (HA and NA). However, in the convalescent patients we found high levels of both CD4+ and CD8+ T-cells directed against conserved core antigens (NP, PA, PB, and M). The results indicate that the antigen targets recognized by the T-cell subsets may vary according to the phase of infection. The apparent low levels of cross-reactive CD8+ T-cells recognizing internal antigens in acute hospitalized patients suggest an important role for this T-cell subset in protective immunity against influenza. [ABSTRACT FROM AUTHOR]

Published

2015

3. Mycobacterial growth inhibition is associated with trained innate immunity.

Author

Joosten, Simone A., van Meijgaarden, Krista E., Arend, Sandra M., Prins, Corine, Oftung, Fredrik, Korsvold, Gro Ellen, Kik, Sandra V., Arts, Rob J. W., van Crevel, Reinout, Netea, Mihai G., Ottenhoff, Tom H. M., Arts, Rob Jw, and Ottenhoff, Tom Hm

Subjects

*MYCOBACTERIUM tuberculosis, *T cells, *MYCOBACTERIUM, *SCURFIN (Protein), *IMMUNE response

Abstract

The lack of defined correlates of protection hampers development of vaccines against tuberculosis (TB). In vitro mycobacterial outgrowth assays are thought to better capture the complexity of the human host/Mycobacterium tuberculosis (Mtb) interaction. Here, we used a mycobacterial growth inhibition assay (MGIA) based on peripheral blood mononuclear cells to investigate the capacity to control outgrowth of bacille Calmette-Guérin (BCG). Interestingly, strong control of BCG outgrowth was observed almost exclusively in individuals with recent exposure to Mtb, but not in (long-term) latent TB infection, and only modestly in BCG vaccinees. Mechanistically, control of mycobacterial outgrowth strongly correlated with the presence of a CD14dim monocyte population, but also required the presence of T cells. The nonclassical monocytes produced CXCL10, and CXCR3 receptor blockade inhibited the capacity to control BCG outgrowth. Expression of CXCR3 splice variants was altered in recently Mtb-exposed individuals. Cytokines previously associated with trained immunity were detected in MGIA supernatants, and CXCL9, CXCL10, and CXCL11 represent new markers of trained immunity. These data indicate that CXCR3 ligands are associated with trained immunity and are critical factors in controlling mycobacterial outgrowth. In conclusion, control of mycobacterial outgrowth early after exposure to Mtb is the result of trained immunity mediated by a CXCL10-producing nonclassical CD14dim monocyte subset. [ABSTRACT FROM AUTHOR]

Published

2018

4. Standardization and validation of assays determining cellular immune responses against influenza

Author

Gijzen, Karlijn, Liu, Wai Ming, Visontai, Ildikó, Oftung, Fredrik, van der Werf, Sylvie, Korsvold, Gro Ellen, Pronk, Inge, Aaberge, Ingeborg S., Tüttő, Anna, Jankovics, Istvan, Jankovics, Mate, Gentleman, Beth, McElhaney, Janet E., and Soethout, Ernst C.

Subjects

*INFLUENZA vaccines, *IMMUNE response, *DRUG efficacy, *BIOMARKERS, *CELL-mediated cytotoxicity, *CYTOKINES, *VIRAL replication, *INTERFERONS

Abstract

Abstract: Influenza vaccine efficacy does not always correlate with humoral immune responses. Recent reports indicate that the cellular immune response also contributes to protection, however robust assays are lacking. We standardized and validated assays for detection of human influenza-specific cellular responses in four international laboratories. The production of granzyme B as marker of T cell-mediated cytotoxicity and release of Th1 and Th2 cytokines were evaluated. The granzyme B and cytokine assays were specific, accurate, precise, and robust. Replicate stimulations with PBMC from the same donors showed an intra-laboratory robustness (coefficient of variation) for quantitation of granzyme B of 33% and for cytokines – including IFN-γ, TNF-α, IL-2, IL-10, IL-4, IL-13, GM-CSF and including the log IFN-γ/IL-10 ratio – of 52%. The inter-laboratory robustness for detection of granzyme B was 29% and for detection of all cytokines was 49%. The assays can now be used for determining cell-mediated immunity and explored as correlates of protection. Moreover, the precision and robustness of these cellular assays allow the reliable detection of cellular responses even in small study populations. [Copyright &y& Elsevier]

Published

2010