Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal

Neonates have a poorly developed immune system. Respiratory pathogens cause disease during early periods of live. Consequently, it is important to develop protective vaccines that induce immunity and immunological memory against respiratory pathogens early in life. Intranasal (i.n.) route could be a...

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Main Authors: Julio A. Balboa, Belkis Romeu, Maribel Cuello, Caridad Zayas, Judith del Campo, Elizabeth González, Reynaldo Acevedo, Miriam Lastre, Osmir Cabrera, Oliver Pérez
Format: Article
Language:English
Published: Finlay Ediciones 2009-08-01
Series:VacciMonitor
Subjects:
Online Access:http://scielo.sld.cu/scielo.php?script=sci_arttext&pid=S1025-028X2009000200009&lng=es&nrm=iso
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spelling doaj-c3762a1b6cd546c3b657a2ac996fd16b2020-11-25T00:00:27ZengFinlay EdicionesVacciMonitor1025-028X1025-02982009-08-011827981Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatalJulio A. Balboa 0Belkis Romeu 1Maribel Cuello2Caridad Zayas3Judith del Campo4Elizabeth González5Reynaldo Acevedo6Miriam Lastre7Osmir Cabrera8 Oliver Pérez 9Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Immunology Department, Research Vice-presidency, Finlay Institute, P.O. Box 16017, Havana, Cuba Neonates have a poorly developed immune system. Respiratory pathogens cause disease during early periods of live. Consequently, it is important to develop protective vaccines that induce immunity and immunological memory against respiratory pathogens early in life. Intranasal (i.n.) route could be an effective via for immunization. Therefore, we explored the effectiveness of AF (Adjuvant Finlay) PL1 (Proteoliposome) from Neisseria meningitidis serogroup B and its derivate Cochleate (AFCo1) by nasal route in neonatal mice. They were immunized i.n. 3 times 7 days apart and anti PL systemic and mucosal antibody response were measured by ELISA. In addition, a prime-boost strategy was used to evaluate the humoral immune response in neonate mice. The 3 doses of AFPL1 or AFCo1 induced significant levels of anti PL IgG antibodies in comparison whit control, but AFCo1 (2017 U/mL) was significantly higher than AFPL1 (1107 U/mL). AFCo1 and AFPL1 induced a predominant Th1 pattern with IgG2a/IgG1 >1 by i.n. immunization and AFCo1 induced a high anti PL IgA saliva response in saliva. Interestingly, one nasally prime at 7 days of born and a memory one boost i.n. dose 9 weeks later with AFCo1 or AFPL1 showed similar specific IgG levels and IgG2a/IgG1 relation than 3 i.n. doses in adult mice. In conclusion, these results represent the first report of neonatal intranasal vaccination using AFCo1 capable to induce systemic and mucosal immunity and priming for memory. http://scielo.sld.cu/scielo.php?script=sci_arttext&pid=S1025-028X2009000200009&lng=es&nrm=isoNeisseria meningitidisOuter membrane vesicleProteoliposomeAFCo1AFPL1Neonatal immunization
collection DOAJ
language English
format Article
sources DOAJ
author Julio A. Balboa
Belkis Romeu
Maribel Cuello
Caridad Zayas
Judith del Campo
Elizabeth González
Reynaldo Acevedo
Miriam Lastre
Osmir Cabrera
Oliver Pérez
spellingShingle Julio A. Balboa
Belkis Romeu
Maribel Cuello
Caridad Zayas
Judith del Campo
Elizabeth González
Reynaldo Acevedo
Miriam Lastre
Osmir Cabrera
Oliver Pérez
Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal
VacciMonitor
Neisseria meningitidis
Outer membrane vesicle
Proteoliposome
AFCo1
AFPL1
Neonatal immunization
author_facet Julio A. Balboa
Belkis Romeu
Maribel Cuello
Caridad Zayas
Judith del Campo
Elizabeth González
Reynaldo Acevedo
Miriam Lastre
Osmir Cabrera
Oliver Pérez
author_sort Julio A. Balboa
title Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal
title_short Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal
title_full Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal
title_fullStr Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal
title_full_unstemmed Inmunización intranasal con AFCo1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal
title_sort inmunización intranasal con afco1 induce respuesta inmune de memoria, sistemica y mucosal en ratones neonatal
publisher Finlay Ediciones
series VacciMonitor
issn 1025-028X
1025-0298
publishDate 2009-08-01
description Neonates have a poorly developed immune system. Respiratory pathogens cause disease during early periods of live. Consequently, it is important to develop protective vaccines that induce immunity and immunological memory against respiratory pathogens early in life. Intranasal (i.n.) route could be an effective via for immunization. Therefore, we explored the effectiveness of AF (Adjuvant Finlay) PL1 (Proteoliposome) from Neisseria meningitidis serogroup B and its derivate Cochleate (AFCo1) by nasal route in neonatal mice. They were immunized i.n. 3 times 7 days apart and anti PL systemic and mucosal antibody response were measured by ELISA. In addition, a prime-boost strategy was used to evaluate the humoral immune response in neonate mice. The 3 doses of AFPL1 or AFCo1 induced significant levels of anti PL IgG antibodies in comparison whit control, but AFCo1 (2017 U/mL) was significantly higher than AFPL1 (1107 U/mL). AFCo1 and AFPL1 induced a predominant Th1 pattern with IgG2a/IgG1 >1 by i.n. immunization and AFCo1 induced a high anti PL IgA saliva response in saliva. Interestingly, one nasally prime at 7 days of born and a memory one boost i.n. dose 9 weeks later with AFCo1 or AFPL1 showed similar specific IgG levels and IgG2a/IgG1 relation than 3 i.n. doses in adult mice. In conclusion, these results represent the first report of neonatal intranasal vaccination using AFCo1 capable to induce systemic and mucosal immunity and priming for memory.
topic Neisseria meningitidis
Outer membrane vesicle
Proteoliposome
AFCo1
AFPL1
Neonatal immunization
url http://scielo.sld.cu/scielo.php?script=sci_arttext&pid=S1025-028X2009000200009&lng=es&nrm=iso
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