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


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.

SUBMITTER: Costa-Pereira C 

PROVIDER: S-EPMC5991646 | biostudies-literature | 2018 Jun

REPOSITORIES: biostudies-literature

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

Costa-Pereira Christiane C   Campi-Azevedo Ana Carolina AC   Coelho-Dos-Reis Jordana Grazziela JG   Peruhype-Magalhães Vanessa V   Araújo Márcio Sobreira Silva MSS   do Vale Antonelli Lis Ribeiro LR   Fonseca Cristina Toscano CT   Lemos Jandira Aparecida JA   Malaquias Luiz Cosme Cote LCC   de Souza Gomes Matheus M   Rodrigues Amaral Laurence L   Rios Maria M   Chancey Caren C   Persi Harold Richard HR   Pereira Jorge Marcelo JM   de Sousa Maia Maria de Lourdes ML   Freire Marcos da Silva MDS   Martins Reinaldo de Menezes RM   Homma Akira A   Simões Marisol M   Yamamura Anna Yoshida AY   Farias Roberto Henrique Guedes RHG   Romano Alessandro Pecego Martins APM   Domingues Carla Magda CM   Tauil Pedro Luiz PL   Vasconcelos Pedro Fernando Costa PFC   Caldas Iramaya Rodrigues IR   Camacho Luiz Antônio LA   Teixeira-Carvalho Andrea A   Martins-Filho Olindo Assis OA  

PLoS neglected tropical diseases 20180607 6


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  ...[more]

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