Your search keyword '"Spertini, François"' showing total 6 results

1. Epitope Mapping and Fine Specificity of Human T and B Cell Responses for Novel Candidate Blood-Stage Malaria Vaccine P27A.

Author

Geiger, Kristina M., Guignard, Daniel, Yang, Che, Bikorimana, Jean-Pierre, Correia, Bruno E., Houard, Sophie, Mkindi, Catherine, Daubenberger, Claudia A., Spertini, François, Corradin, Giampietro, and Audran, Régine

Subjects

MALARIA vaccines, HUMAN T cells, PLASMODIUM falciparum, B cells, T cells

Abstract

P27A is a novel synthetic malaria vaccine candidate derived from the blood stage Plasmodium falciparum protein Trophozoite Exported Protein 1 (TEX1/PFF0165c). In phase 1a/1b clinical trials in malaria unexposed adults in Switzerland and in malaria pre-exposed adults in Tanzania, P27A formulated with Alhydrogel and GLA-SE adjuvants induced antigen-specific antibodies and T-cell activity. The GLA-SE adjuvant induced significantly stronger humoral responses than the Alhydrogel adjuvant. Groups of pre-exposed and unexposed subjects received identical vaccine formulations, which supported the comparison of the cellular and humoral response to P27A in terms of fine specificity and affinity for populations and adjuvants. Globally, fine specificity of the T and B cell responses exhibited preferred recognized sequences and did not highlight major differences between adjuvants or populations. Affinity of anti-P27A antibodies was around 10−8 M in all groups. Pre-exposed volunteers presented anti-P27A with higher affinity than unexposed volunteers. Increasing the dose of GLA-SE from 2.5 to 5 μg in pre-exposed volunteers improved anti-P27A affinity and decreased the number of recognized epitopes. These results indicate a higher maturation of the humoral response in pre-exposed volunteers, particularly when immunized with P27A formulated with 5 μg GLA-SE. [ABSTRACT FROM AUTHOR]

Published

2020

2. Results of the phase I open label clinical trial SAKK 06/14 assessing safety of intravesical instillation of VPM1002BC, a recombinant mycobacterium Bacillus Calmette Guérin (BCG), in patients with non-muscle invasive bladder cancer and previous failure of conventional BCG therapy

Author

Rentsch, Cyrill A., Bosshard, Piet, Mayor, Grégoire, Rieken, Malte, Püschel, Heike, Wirth, Grégory, Cathomas, Richard, Parzmair, Gerald P., Grode, Leander, Eisele, Bernd, Sharma, Hitt, Gupta, Manish, Gairola, Sunil, Shaligram, Umesh, Goldenberger, Daniel, Spertini, François, Audran, Régine, Enoiu, Milica, Berardi, Simona, and Hayoz, Stefanie

Subjects

MYCOBACTERIUM, CLINICAL trials, INTERSTITIAL cystitis, BLADDER cancer, T cells, GRANULOCYTE-macrophage colony-stimulating factor, PATIENT safety, IMMUNE response

Abstract

Background: VPM1002BC is a modified mycobacterium Bacillus Calmette Guérin (BCG) for the treatment of non-muscle invasive bladder cancer (NMIBC). The genetic modifications are expected to result in better immunogenicity and less side effects. We report on patient safety and immunology of the first intravesical application of VPM1002BC in human. Methods: Six patients with BCG failure received a treatment of 6 weekly instillations with VPM1002BC. Patients were monitored for adverse events (AE), excretion of VPM1002BC and cytokines, respectively. Results: No DLT (dose limiting toxicity) occurred during the DLT-period. No grade ≥3 AEs occurred. Excretion of VPM1002BC in the urine was limited to less than 24 hours. Plasma levels of TNFα significantly increased after treatment and blood-derived CD4+ T cells stimulated with PPD demonstrated significantly increased intracellular GM-CSF and IFN expression. Conclusion: The intravesical application of VPM1002BC is safe and well tolerated by patients and results in a potential Th1 weighted immune response. [ABSTRACT FROM AUTHOR]

Published

2020

3. The candidate tuberculosis vaccine Mtb72F/AS02 in PPD positive adults: A randomized controlled phase I/II study.

Author

Spertini, François, Audran, Régine, Lurati, Floriana, Ofori-Anyinam, Opokua, Zysset, Frédéric, Vandepapelière, Pierre, Moris, Philippe, Demoitié, Marie-Ange, Mettens, Pascal, Vinals, Carlota, Vastiau, Ilse, Jongert, Erik, Cohen, Joe, and Ballou, W. Ripley

Subjects

TUBERCULOSIS prevention, TUBERCULOSIS vaccines, CHEMOPREVENTION, T cells, DISEASE complications, RANDOMIZED controlled trials

Abstract

Summary: Prevention of tuberculosis (TB) through vaccination would substantially reduce the global TB burden. Mtb72F/AS02 is a candidate TB vaccine shown to be immunogenic and well tolerated in PPD-negative adults. We evaluated the safety and immunogenicity of Mtb72F/AS02 in Mycobacterium-primed adults (BCG-vaccinated, or infected adults who had received post-exposure chemoprophylaxis or treatment for pulmonary TB disease). In this observer-blind controlled trial, 20 BCG-vaccinated adults and 18 adults previously infected with Mycobacterium tuberculosis (Mtb), were randomized 3:1 to receive three doses of Mtb72F/AS02 or AS02 at one-month intervals, and followed for 6 months post third vaccination. Mtb72F/AS02 was well tolerated in BCG-vaccinated adults, and tended to be more reactogenic in Mtb-infected adults. Adverse events were mainly self-limiting, resolving without sequelae. No serious adverse events were reported. The adverse events in Mtb72F/AS02 vaccinees were not clearly associated with vaccine-induced responses (as assessed by proinflammatory cytokines, total IgE and C-reactive protein levels). No Th2 T-cell responses, or vaccine-induced T-cell responses to Mtb antigens (CFP-10/PPD/ESAT-6) were detected by ICS. In both cohorts, Mtb72F/AS02 induced persistent polyfunctional Mtb72F-specific CD4+ T-cell responses and anti-Mtb72F humoral responses. IFN-γ was detectable in serum one day post each vaccination. Further evaluation of the candidate vaccine, Mtb72F/AS02, is warranted. Trial registration: ClinicalTrials.gov identifier: NCT00146744. [ABSTRACT FROM AUTHOR]

Published

2013

4. CD4+CD25−mTGFβ+ T cells induced by nasal application of ovalbumin transfer tolerance in a therapeutic model of asthma.

Author

Pellaton-Longaretti, Céline, Boudousquié, Caroline, Barbier, Nathalie, Barbey, Catherine, Argiroffo, Constance Barazzone, Donati, Yves, Sauty, Alain, and Spertini, François

Subjects

INTRANASAL medication, T cells, ASTHMA, TRANSFORMING growth factors, IMMUNOLOGICAL tolerance, LABORATORY mice, CELL proliferation, INFLAMMATION, GENETIC regulation

Abstract

Background: Intranasal administration of high amount of allergen was shown to induce tolerance and to reverse the allergic phenotype. However, mechanisms of tolerance induction via the mucosal route are still unclear. Objectives: To characterize the therapeutic effects of intranasal application of ovalbumin (OVA) in a mouse model of bronchial inflammation as well as the cellular and molecular mechanisms leading to protection upon re-exposure to allergen. Methods: After induction of bronchial inflammation, mice were treated intranasally with OVA and re-exposed to OVA aerosols 10 days later. Bronchoalveolar lavage fluid (BALF), T cell proliferation and cytokine secretion were examined. The respective role of CD4+CD25+ and CD4+CD25− T cells in the induction of tolerance was analysed. Results: Intranasal treatment with OVA drastically reduced inflammatory cell recruitment into BALF and bronchial hyperresponsiveness upon re-exposure to allergen. Both OVA- specific-proliferation of T cells, Th1 and Th2 cytokine production from lung and bronchial lymph nodes were inhibited. Transfer of CD4+CD25− T cells, which strongly expressed membrane-bound transforming growth factor β (mTGFβ), from tolerized mice protected asthmatic recipient mice from subsequent aerosol challenges. The presence of CD4+CD25+(Foxp3+) T cells during the process of tolerization was indispensable to CD4+CD25− T cells to acquire regulatory properties. Whereas the presence of IL-10 appeared dispensable in this model, the suppression of CD4+CD25−mTGFβ+ T cells in transfer experiments significantly impaired the down-regulation of airways inflammation. Conclusion: Nasal application of OVA in established asthma led to the induction of CD4+CD25−mTGFβ+ T cells with regulatory properties, able to confer protection upon allergen re-exposure. [ABSTRACT FROM AUTHOR]

Published

2011

5. The Synthetic Plasmodium falciparum Circumsporozoite Peptide PfCS102 as a Malaria Vaccine Candidate: A Randomized Controlled Phase I Trial.

Author

Audran, Régine, Lurati-Ruiz, Floriana, Genton, Blaise, Blythman, Hildur E., Ofori-Anyinam, Opokua, Reymond, Christophe, Corradin, Giampietro, and Spertini, François

Subjects

PLASMODIUM falciparum, MALARIA vaccines, T cells, CUTANEOUS manifestations of general diseases, IMMUNIZATION, PROTOZOAN vaccines, CELLULAR immunity, PREVENTION of communicable diseases, RANDOMIZED controlled trials

Abstract

Background: Fully efficient vaccines against malaria pre-erythrocytic stage are still lacking. The objective of this dose/ adjuvant-finding study was to evaluate the safety, reactogenicity and immunogenicity of a vaccine candidate based on a peptide spanning the C-terminal region of Plasmodium falciparum circumsporozoite protein (PfCS102) in malaria naive adults. Methodology and Principal Findings: Thirty-six healthy malaria-naive adults were randomly distributed into three dose blocks (10, 30 and 100 mg) and vaccinated with PfCS102 in combination with either Montanide ISA 720 or GSK proprietary Adjuvant System AS02A at days 0, 60, and 180. Primary end-point (safety and reactogenicity) was based on the frequency of adverse events (AE) and of abnormal biological safety tests; secondary-end point (immunogenicity) on P. falciparum specific cell-mediated immunity and antibody response before and after immunization. The two adjuvant formulations were well tolerated and their safety profile was good. Most AEs were local and, when systemic, involved mainly fatigue and headache. Half the volunteers in AS02A groups experienced severe AEs (mainly erythema). After the third injection, 34 of 35 volunteers developed anti-PfCS102 and anti-sporozoite antibodies, and 28 of 35 demonstrated T-cell proliferative responses and IFN-γ production. Five of 22 HLA-A2 and HLA-A3 volunteers displayed PfCS102 specific IFN-γ secreting CD8+ T cell responses. Responses were only marginally boosted after the 3rd vaccination and remained stable for 6 months. For both adjuvants, the dose of 10 μg was less immunogenic in comparison to 30 and 100 mg that induced similar responses. AS02A formulations with 30 μg or 100 μg PfCS102 induced about 10-folds higher antibody and IFN-γ responses than Montanide formulations. Conclusions/Significance: PfCS102 peptide was safe and highly immunogenic, allowing the design of more advanced trials to test its potential for protection. Two or three immunizations with a dose of 30 μg formulated with AS02A appeared the most appropriate choice for such studies. Trial Registration: Swissmedic.ch 2002 DR 1227 [ABSTRACT FROM AUTHOR]

Published

2009

6. Epitope-specific crosslinking of CD45 down-regulates membrane-associated tyrosine phosphatase activity and triggers early signalling events in human activated T cells.

Author

Spertini, François, Perret-Menoud, Veronique, Barbier, Nathalie, Chatila, Talal, Barbey, Catherine, and Corthesy, Blaise

Subjects

*PROTEIN-tyrosine phosphatase, *T cells, *CROSSLINKING (Polymerization), *GENE expression, *TUMOR necrosis factors, *CELL membranes

Abstract

CD45 engagement by monoclonal antibodies on human activated T cells triggers tumour necrosis factor-α (TNF-α) gene transcription in an epitope-specific manner. To dissect the early signalling events leading to TNF-α gene expression, we established that CD45 crosslinking resulted in tyrosine phosphorylation of p56lck, ZAP-70, CD3-ζ, LAT and Vav. This was accompanied by down-regulation of membrane-associated protein tyrosine phosphatase activity in the absence of demonstration of enhanced p56lck, p72sykand ZAP-70 kinase activity, which remained constitutive. These early events eventually triggered an intracellular Ca2+ rise and phosphoinositide turnover. We conclude that down-regulation of membrane-associated tyrosine phosphatase activity by CD45 extracytoplasmic domain multimerization led, in an epitope-specific fashion, to unopposed tyrosine kinase activity and to the activation of the T-cell receptor/CD3 complex signalling cascade, resulting in TNF-α gene expression. This model strongly suggests that CD45 extracytoplasmic tail multimerization may contribute to the modulation T-cell functions. [ABSTRACT FROM AUTHOR]

Published

2004