Your search keyword '"Costa-Pereira, Christiane"' showing total 5 results

1. Multi-parameter approach to evaluate the timing of memory status after 17DD-YF primary vaccination.

Author

Costa-Pereira C, Campi-Azevedo AC, Coelho-Dos-Reis JG, Peruhype-Magalhães V, Araújo MSS, do Vale Antonelli LR, Fonseca CT, Lemos JA, Malaquias LCC, de Souza Gomes M, Rodrigues Amaral L, Rios M, Chancey C, Persi HR, Pereira JM, de Sousa Maia ML, Freire MDS, Martins RM, Homma A, Simões M, Yamamura AY, Farias RHG, Romano APM, Domingues CM, Tauil PL, Vasconcelos PFC, Caldas IR, Camacho LA, Teixeira-Carvalho A, and Martins-Filho OA

Subjects

Adolescent, Adult, Aged, B-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Cytokines blood, Humans, Male, Middle Aged, Time Factors, Yellow Fever immunology, Yellow Fever virology, Young Adult, Antibodies, Viral blood, Biomarkers blood, Vaccination, Yellow Fever prevention & control, Yellow Fever Vaccine immunology, Yellow fever virus immunology

Abstract

In this investigation, machine-enhanced techniques were applied to bring about scientific insights to identify a minimum set of phenotypic/functional memory-related biomarkers for post-vaccination follow-up upon yellow fever (YF) vaccination. For this purpose, memory status of circulating T-cells (Naïve/early-effector/Central-Memory/Effector-Memory) and B-cells (Naïve/non-Classical-Memory/Classical-Memory) along with the cytokine profile (IFN/TNF/IL-5/IL-10) were monitored before-NV(day0) and at distinct time-points after 17DD-YF primary vaccination-PV(day30-45); PV(year1-9) and PV(year10-11). A set of biomarkers (eEfCD4; EMCD4; CMCD19; EMCD8; IFNCD4; IL-5CD8; TNFCD4; IFNCD8; TNFCD8; IL-5CD19; IL-5CD4) were observed in PV(day30-45), but not in NV(day0), with most of them still observed in PV(year1-9). Deficiencies of phenotypic/functional biomarkers were observed in NV(day0), while total lack of memory-related attributes was observed in PV(year10-11), regardless of the age at primary vaccination. Venn-diagram analysis pre-selected 10 attributes (eEfCD4, EMCD4, CMCD19, EMCD8, IFNCD4, IL-5CD8, TNFCD4, IFNCD8, TNFCD8 and IL-5CD4), of which the overall mean presented moderate accuracy to discriminate PV(day30-45)&PV(year1-9) from NV(day0)&PV(year10-11). Multi-parameter approaches and decision-tree algorithms defined the EMCD8 and IL-5CD4 attributes as the top-two predictors with moderated performance. Together with the PRNT titers, the top-two biomarkers led to a resultant memory status observed in 80% and 51% of volunteers in PV(day30-45) and PV(year1-9), contrasting with 0% and 29% found in NV(day0) and PV(year10-11), respectively. The deficiency of memory-related attributes observed at PV(year10-11) underscores the conspicuous time-dependent decrease of resultant memory following17DD-YF primary vaccination that could be useful to monitor potential correlates of protection in areas under risk of YF transmission., Competing Interests: Seven participants of this study (MS, MSF, AMYY, AH, RMM, RHGF, MLSM) are employees at the 17DD-YF vaccine manufacturer (Bio-Manguinhos, Fundação Oswaldo Cruz), and nine participants work in other units of Fundação Oswaldo Cruz (ACCA, MSSA, VPM, LRVA, CTF, LABC, IRC, ATC and OAMF). Bias from competing interest was prevented by: (1) one collaboration with a general clinical Physician (HRP) from Brazilian Army, expert in infectious disease; (2) one general clinical Nurse (JACL) expert in vaccine epidemiological vigilance from State Health Department; (3) three Immunologists (LCCM) from Brazilian Research Academy and (MR and CC) from United States Department of Health; and (5) two independent professionals working as PhD student (CCP) or Post-Doc Researchers (JGCR) in the field of infectious diseases. (6) two authors (MSG and LRA) from the Universidade Federal de Alfenas contributed to bioinformatics analysis (decision tree algorithm). The FIOCRUZ extramural coworkers contributed with critical overview of the studystrategy, immunization of volunteers as well as medical care, blood sample collection, blind sample handling and processing, data collection, statistical analysis and data interpretation. The views and opinions expressed here are those of the authors and do not represent the official position of the US FDA.

Published

2018

2. Heparin removal by ecteola-cellulose pre-treatment enables the use of plasma samples for accurate measurement of anti-Yellow fever virus neutralizing antibodies.

Author

Campi-Azevedo AC, Peruhype-Magalhães V, Coelho-Dos-Reis JG, Costa-Pereira C, Yamamura AY, Lima SMB, Simões M, Campos FMF, de Castro Zacche Tonini A, Lemos EM, Brum RC, de Noronha TG, Freire MS, Maia MLS, Camacho LAB, Rios M, Chancey C, Romano A, Domingues CM, Teixeira-Carvalho A, and Martins-Filho OA

Subjects

Adolescent, Adult, Aged, Biomarkers blood, Cellulose chemistry, Child, Child, Preschool, Female, Humans, Infant, Male, Middle Aged, Predictive Value of Tests, Reproducibility of Results, Viral Plaque Assay, Yellow Fever blood, Yellow Fever diagnosis, Yellow Fever virology, Young Adult, Antibodies, Neutralizing blood, Antibodies, Viral blood, Anticoagulants blood, Blood Specimen Collection methods, Cellulose analogs & derivatives, Drug Monitoring methods, Heparin blood, Neutralization Tests, Vaccination, Yellow Fever prevention & control, Yellow Fever Vaccine administration & dosage, Yellow fever virus immunology

Abstract

Technological innovations in vaccinology have recently contributed to bring about novel insights for the vaccine-induced immune response. While the current protocols that use peripheral blood samples may provide abundant data, a range of distinct components of whole blood samples are required and the different anticoagulant systems employed may impair some properties of the biological sample and interfere with functional assays. Although the interference of heparin in functional assays for viral neutralizing antibodies such as the functional plaque-reduction neutralization test (PRNT), considered the gold-standard method to assess and monitor the protective immunity induced by the Yellow fever virus (YFV) vaccine, has been well characterized, the development of pre-analytical treatments is still required for the establishment of optimized protocols. The present study intended to optimize and evaluate the performance of pre-analytical treatment of heparin-collected blood samples with ecteola-cellulose (ECT) to provide accurate measurement of anti-YFV neutralizing antibodies, by PRNT. The study was designed in three steps, including: I. Problem statement; II. Pre-analytical steps; III. Analytical steps. Data confirmed the interference of heparin on PRNT reactivity in a dose-responsive fashion. Distinct sets of conditions for ECT pre-treatment were tested to optimize the heparin removal. The optimized protocol was pre-validated to determine the effectiveness of heparin plasma:ECT treatment to restore the PRNT titers as compared to serum samples. The validation and comparative performance was carried out by using a large range of serum vs heparin plasma:ECT 1:2 paired samples obtained from unvaccinated and 17DD-YFV primary vaccinated subjects. Altogether, the findings support the use of heparin plasma:ECT samples for accurate measurement of anti-YFV neutralizing antibodies., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

3. Vaccination against canine leishmaniosis increases the phagocytic activity, nitric oxide production and expression of cell activation/migration molecules in neutrophils and monocytes.

Author

Moreira ML, Costa-Pereira C, Alves ML, Marteleto BH, Ribeiro VM, Peruhype-Magalhães V, Giunchetti RC, Martins-Filho OA, and Araújo MS

Subjects

Animals, Antibodies, Protozoan blood, Brazil, Cytokines genetics, Dog Diseases immunology, Dog Diseases prevention & control, Dogs, Female, Gene Expression Regulation immunology, Leishmaniasis, Visceral immunology, Leishmaniasis, Visceral prevention & control, Leishmaniasis, Visceral veterinary, Male, Leishmaniasis Vaccines immunology, Monocytes immunology, Neutrophils immunology, Nitric Oxide metabolism, Phagocytosis immunology, Vaccination veterinary

Abstract

Visceral leishmaniasis (VL) is transmitted by phlebotomine sandfly vectors and domestic dogs serve as a reservoir. The elimination of seropositive dogs has been a recommended strategy for managing the disease in Brazil. A protective canine vaccine would be an important tool for controlling the disease, reducing the parasites available to sandfly vectors and, consequently, reducing the number of human VL cases. Leishmune(®) is an anti-canine Leishmaniosis (VL Canine) vaccine produced by Zoetis (Pfizer, Brazil) that was commercially available in Brazil until 2014. The main goal of the present study was to investigate the protective immunological events induced by vaccination with Leishmune(®) in the time frame of one year. Healthy, non-vaccinated dogs and dogs of 1, 6 and 10 months post-vaccination were evaluated. Results showed that Leishmune(®) induced an increase in phagocytic activity of neutrophils and monocytes and also increased NO production. Immunological events were correlated with functional responses, as high levels of IgG and an increase of the receptor Fcγ were detected. Vaccination induced an increased expression of TLR (2, 4, 5, 9), integrin (CD29, CD49f), activation (MHCII) and co-stimulatory (CD80, CD81) molecules by neutrophils and monocytes. Vaccination led to decrease of IL-4 and an increase of IL-8 production by monocytes and higher IFN-γ and IL-17 production by T-cells. The results suggested that Leishmune(®) was able to induce a long-lasting change in immune response, mediated by supportive immunological events that may be participating in protective immunity against CL., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

4. 17DD Yellow Fever Revaccination and Heightened Long-Term Immunity in Populations of Disease-Endemic Areas, Brazil

Author

Campi-Azevedo, Ana Carolina, Peruhype-Magalhaes, Vanessa, Coelho-dos-Reis, Jordana Grazziela, Antonelli, Lis Ribeiro, Costa-Pereira, Christiane, Speziali, Elaine, Reis, Laise Rodrigues, Lemos, Jandira Aparecida, Ribeiro, Jose Geraldo Leite, Camacho, Luiz Antonio Bastos, de Lourdes de Sousa Maia, Maria, de Lima, Sheila Maria Barbosa, Simoes, Marisol, de Menezes Martins, Reinaldo, Homma, Akira, Malaquias, Luiz Cosme Cota, Tauil, Pedro Luiz, Vasconcelos, Pedro Fernando Costa, Romano, Alessandro Pecego Martins, Domingues, Carla Magda, Teixeira-Carvalho, Andrea, and Martins-Filho, Olindo Assis

Subjects

Vaccines, Biological response modifiers, Yellow fever, B cells, Vaccination, Interferon, Antibodies, T cells, Memory, Immune response, Health, World Health Organization

Abstract

Yellow fever (YF) vaccination is recommended for persons living in YF-endemic areas as the most effective strategy to reduce the risk for infection (1). The 17D and 17DD live attenuated [...]

Published

2019

5. Short-Lived Immunity After 17DD Yellow Fever Single Dose Indicates That Booster Vaccination May Be Required to Guarantee Protective Immunity in Children.

Author

Campi-Azevedo, Ana Carolina, Reis, Laise Rodrigues, Peruhype-Magalhães, Vanessa, Coelho-dos-Reis, Jordana Grazziela, Antonelli, Lis Ribeiro, Fonseca, Cristina Toscano, Costa-Pereira, Christiane, Souza-Fagundes, Elaine Maria, Costa-Rocha, Ismael Artur da, Mambrini, Juliana Vaz de Melo, Lemos, Jandira Aparecida Campos, Ribeiro, José Geraldo Leite, Caldas, Iramaya Rodrigues, Camacho, Luiz Antônio Bastos, Maia, Maria de Lourdes de Sousa, de Noronha, Tatiana Guimarães, de Lima, Sheila Maria Barbosa, Simões, Marisol, Freire, Marcos da Silva, and Martins, Reinaldo de Menezes

Subjects

YELLOW fever, VACCINATION, LONG-term memory, CELLULAR immunity, PSYCHONEUROIMMUNOLOGY

Abstract

The Yellow Fever (YF) vaccination is recommended for people living in endemic areas and represents the most effective strategy to reduce the risk of infection. Previous studies have warned that booster regimens should be considered to guarantee the long-term persistence of 17DD-YF-specific memory components in adults living in areas with YF-virus circulation. Considering the lower seroconversion rates observed in children (9–12 months of age) as compared to adults, this study was designed in order to access the duration of immunity in single-dose vaccinated children in a 10-years cross-sectional time-span. The levels of neutralizing antibodies (PRNT) and the phenotypic/functional memory status of T and B-cells were measured at a baseline, 30–45 days, 1, 2, 4, 7, and 10 years following primary vaccination. The results revealed that a single dose induced 85% of seropositivity at 30–45 days and a progressive time-dependent decrease was observed as early as 2 years and declines toward critical values (below 60%) at time-spans of ≥4-years. Moreover, short-lived YF-specific cellular immunity, mediated by memory T and B-cells was also observed after 4-years. Predicted probability and resultant memory analysis emphasize that correlates of protection (PRNT; effector memory CD8+ T-cells; non-classical memory B-cells) wane to critical values within ≥4-years after primary vaccination. Together, these results clearly demonstrate the decline of 17DD-YF-specific memory response along time in children primarily vaccinated at 9–12 months of age and support the need of booster regimen to guarantee the long-term persistence of memory components for children living in areas with high risk of YF transmission. [ABSTRACT FROM AUTHOR]

Published

2019