Your search keyword '"Romero, Jackeline"' showing total 6 results

1. Peptide vaccination.

Author

Meraldi V, Romero JF, and Corradin G

Subjects

Animals, Antigens, Protozoan isolation & purification, Chromatography, Gel methods, Chromatography, High Pressure Liquid methods, Injections, Intraperitoneal, Malaria prevention & control, Mice, Peptides isolation & purification, Quality Control, Spectrophotometry methods, Antigens, Protozoan immunology, Malaria immunology, Malaria Vaccines administration & dosage, Malaria Vaccines standards, Peptides immunology, Plasmodium immunology

Published

2002

2. CSP-A Model for In Vivo Presentation of Plasmodium berghei Sporozoite Antigens by Hepatocytes.

Author

Balam, Saidou, Romero, Jackeline F., Bongfen, Silayuv E., Guillaume, Philippe, and Corradin, Giampietro

Subjects

*PLASMODIUM berghei, *ANTIGENS, *IMMUNITY, *PLASMODIUM, *T cells, *LYMPHOCYTES

Abstract

One target of protective immunity against the Plasmodium liver stage in BALB/c mice is represented by the circumsporozoite protein (CSP), and mainly involves its recognition by IFN-γ producing specific CD8+T-cells. In a previous in vitro study we showed that primary hepatocytes from BALB/c mice process Plasmodium berghei (Pb) CSP (PbCSP) and present CSP-derived peptides to specific H-2kd restricted CD8+T-cells with subsequent killing of the presenting cells. We now extend these observations to an in vivo infection model in which infected hepatocytes and antigen specific T-cell clones are transferred into recipient mice inducing protection from sporozoite (SPZ) challenge. In addition, using a similar protocol, we suggest the capacity of hepatocytes in priming of naïve T-cells to provide protection, as further confirmed by induction of protection after depletion of cross-presenting dendritic cells (DCs) by cytochrome c (cyt c) treatment or using traversal deficient parasites. Our results clearly show that hepatocytes present Plasmodium CSP to specific-primed CD8+T-cells, and could also prime naïve T-cells, leading to protection from infection. These results could contribute to a better understanding of liver stage immune response and design of malaria vaccines. [ABSTRACT FROM AUTHOR]

Published

2012

3. Malarial Hemozoin Is a Nalp3 Inflammasome Activating Danger Signal.

Author

Dostert, Catherine, Guarda, Greta, Romero, Jackeline F., Menu, Philippe, Gross, Olaf, Tardivel, Aubry, Suva, Mario-Luca, Stehle, Jean-Christophe, Kopf, Manfred, Stamenkovic, Ivan, Corradin, Giampietro, and Tschopp, Jurg

Subjects

MALARIA, FEVER, PLASMODIUM, HEMOGLOBINS, ERYTHROCYTE disorders, PERITONITIS, CEREBRAL malaria, HEMATOLOGY, PATHOLOGY

Abstract

Background: Characteristic symptoms of malaria include recurrent fever attacks and neurodegeneration, signs that are also found in patients with a hyperactive Nalp3 inflammasome. Plasmodium species produce a crystal called hemozoin that is generated by detoxification of heme after hemoglobin degradation in infected red blood cells. Thus, we hypothesized that hemozoin could activate the Nalp3 inflammasome, due to its particulate nature reminiscent of other inflammasomeactivating agents. Methodology/Principal Findings: We found that hemozoin acts as a proinflammatory danger signal that activates the Nalp3 inflammasome, causing the release of IL-1β. Similar to other Nalp3-activating particles, hemozoin activity is blocked by inhibiting phagocytosis, K+ efflux and NADPH oxidase. In vivo, intraperitoneal injection of hemozoin results in acute peritonitis, which is impaired in Nalp3-, caspase-1- and IL-1R-deficient mice. Likewise, the pathogenesis of cerebral malaria is dampened in Nalp3-deficient mice infected with Plasmodium berghei sporozoites, while parasitemia remains unchanged. Significance/Conclusions: The potent pro-inflammatory effect of hemozoin through inflammasome activation may possibly be implicated in plasmodium-associated pathologies such as cerebral malaria. [ABSTRACT FROM AUTHOR]

Published

2009

4. Intranasal administration of the synthetic polypeptide from the C-terminus of the circumsporozoite protein of Plasmodium berghei with the modified heat-labile toxin of Escherichia coli (LTK63) induces a complete protection against malaria challenge

Author

Romero, Jackeline F., Ciabattini, Annalisa, Guillaume, Philippe, Frank, Geraldine, Ruggiero, Paolo, Pettini, Elena, Del Giudice, Giuseppe, Medaglini, Donata, and Corradin, Giampietro

Subjects

*INTRANASAL medication, *POLYPEPTIDES, *BACTERIAL proteins, *PLASMODIUM, *BACTERIAL toxins, *MALARIA vaccines, *ESCHERICHIA coli, *VACCINATION of children

Abstract

Abstract: Needle-free procedures are very attractive ways to deliver vaccines because they diminish the risk of contamination and may reduce local reactions, pain or pain fear especially in young children with a consequence of increasing the vaccination coverage for the whole population. For this purpose, the possible development of a mucosal malaria vaccine was investigated. Intranasal immunization was performed in BALB/c mice using a well-studied Plasmodium berghei model antigen derived from the circumsporozoite protein with the modified heat-labile toxin of Escherichia coli (LTK63), which is devoid of any enzymatic activity compared to the wild type form. Here, we show that intranasal administration of the two compounds activates the T and B cell immune response locally and systemically. In addition, a total protection of mice is obtained upon a challenge with live sporozoites. [Copyright &y& Elsevier]

Published

2009

5. CD1d-restricted NK T cells are dispensable for specific antibody responses and protective immunity against liver stage malaria infection in mice.

Author

Romero, Jackeline F., Eberl, Gérard, Robson Macdonald, H., and Corradin, Giampietro

Subjects

*PLASMODIUM, *MALARIA, *MOUSE diseases, *KILLER cells, *T cells, *VACCINATION

Abstract

Immunization with a single dose of irradiated sporozoites is sufficient to induce protection against malaria in wild-type mice. Although this protection is classically attributed to conventional CD4+ and CD8+ T cells, several recent reports have suggested an important role for CD1-restricted NK T cells in immunity to malaria. In this study, we directly compared the ability of C57BL/6 wild-type and CD1-deficient mice to mount a protective immune response against Plasmodium berghei sporozoites. Our data indicate that CD1-restricted NK T cells are not required for protection in this model system. Moreover, specific IgG antibody responses to the P. berghei circumsporozoite repeat sequence were also unaffected by CD1 deficiency. Collectively, our data demonstrate that CD1-restricted NK T cells are dispensable for protective immunity to liver stage P. berghei infection. [ABSTRACT FROM AUTHOR]

Published

2001

6. OM-174, a new adjuvant with a potential for human use, induces a protective response when administered with the synthetic C-terminal fragment 242–310 from the circumsporozoite protein of Plasmodium berghei

Author

Meraldi, Valentin, Audran, Régine, Romero, Jackeline F., Brossard, Vincent, Bauer, Jacques, López, José Alejandro, and Corradin, Giampietro

Subjects

*ESCHERICHIA coli, *PLASMODIUM

Abstract

The goal of this project was the evaluation of a novel immunomodulatory adjuvant for human use, OM-174, which is a soluble adjuvant derived from Escherichia coli lipid A. For this study, we used a synthetic peptide, known for its safety and reproducibility and the murine model of BALB/c mice. The long peptide (PbCS 242–310) used corresponds to the C-terminal region of the circumsporozoite protein (CSP) that is the major protein on the surface of Plasmodium sporozoites. Subcutaneous injections of PbCS 242–310 in combination with soluble adjuvant OM-174 induced long lasting peptide-specific antibody titres comparable to those obtained by immunization with incomplete Freund’s adjuvant (IFA). The ex vivo evaluation of the CD8+ T cell response by IFN-γ ELISPOT assay revealed that the injection of polypeptide with OM-174 adjuvant induced, compared to IFA, a similar and an eight-fold increased frequency of peptide-specific lymphocytes in the draining lymph-nodes and in the spleen, respectively. The CD8+ T-cells are specific for the sequence PbCS 245–253, a well-known H-2Kd-restricted CTL epitope, and are cytotoxic as shown in a chromium release assay. Immunization of BALB/c mice with this polypeptide in combination with adjuvant OM-174 conferred a protection after challenge with live Plasmodium berghei sporozoites.The strong antibody and CTL responses observed to a synthetic peptide in mice, the safety profile of the adjuvant and its extensive physico-chemical characterization suggest that OM-174 has a potential use in vaccine formulations for humans. [Copyright &y& Elsevier]

Published

2003