Heterologous prime-boost strategy to immunize very young infants against measles: Pre-clinical studies in rhesus macaques

M. F. Pasetti; A. Resendiz-Albor; K. Ramirez; R. Stout; M. Papania; R. J. Adams; F. P. Polack; B. J. Ward; D. Burt; S. Chabot; J. Ulmer; E. M. Barry; M. M. Levine

doi:10.1038/sj.clpt.6100420

Heterologous prime-boost strategy to immunize very young infants against measles: Pre-clinical studies in rhesus macaques

M. F. Pasetti, A. Resendiz-Albor, K. Ramirez, R. Stout, M. Papania, R. J. Adams, F. P. Polack, B. J. Ward, D. Burt, S. Chabot, J. Ulmer, E. M. Barry, M. M. Levine

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Resumen

Infants in developing countries are at high risk of developing severe clinical measles if they become infected during the "window of vulnerability" (age 4-9 months), when declining maternal antibodies do not protect against wild virus, yet impede successful immunization by attenuated measles vaccine. We developed two Sindbis replicon-based DNA vaccines expressing measles virus hemagglutinin and fusion protein with the goal of priming young infants to respond safely and effectively to subsequent boosting with attenuated measles vaccine. Intradermal prime with DNA vaccines by needle-free injection followed by aerosol or parenteral boost with licensed measles vaccine was well tolerated by juvenile and young infant rhesus macaques, and protected against clinical measles and viremia on wild-type virus challenge. A proteosome-measles vaccine administered alone (three doses) or as a boost following DNA vaccine priming was also safe and protective. These promising results pave the way for clinical trials to assess this prime-boost strategy.

Idioma original	Inglés
Páginas (desde-hasta)	672-685
Número de páginas	14
Publicación	Clinical Pharmacology & Therapeutics
Volumen	82
N.º	6
DOI	https://doi.org/10.1038/sj.clpt.6100420
Estado	Publicada - dic. 2007
Publicado de forma externa	Sí

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Pasetti, M. F., Resendiz-Albor, A., Ramirez, K., Stout, R., Papania, M., Adams, R. J., Polack, F. P., Ward, B. J., Burt, D., Chabot, S., Ulmer, J., Barry, E. M., & Levine, M. M. (2007). Heterologous prime-boost strategy to immunize very young infants against measles: Pre-clinical studies in rhesus macaques. Clinical Pharmacology & Therapeutics, 82(6), 672-685. https://doi.org/10.1038/sj.clpt.6100420

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title = "Heterologous prime-boost strategy to immunize very young infants against measles: Pre-clinical studies in rhesus macaques",

abstract = "Infants in developing countries are at high risk of developing severe clinical measles if they become infected during the {"}window of vulnerability{"} (age 4-9 months), when declining maternal antibodies do not protect against wild virus, yet impede successful immunization by attenuated measles vaccine. We developed two Sindbis replicon-based DNA vaccines expressing measles virus hemagglutinin and fusion protein with the goal of priming young infants to respond safely and effectively to subsequent boosting with attenuated measles vaccine. Intradermal prime with DNA vaccines by needle-free injection followed by aerosol or parenteral boost with licensed measles vaccine was well tolerated by juvenile and young infant rhesus macaques, and protected against clinical measles and viremia on wild-type virus challenge. A proteosome-measles vaccine administered alone (three doses) or as a boost following DNA vaccine priming was also safe and protective. These promising results pave the way for clinical trials to assess this prime-boost strategy.",

author = "Pasetti, {M. F.} and A. Resendiz-Albor and K. Ramirez and R. Stout and M. Papania and Adams, {R. J.} and Polack, {F. P.} and Ward, {B. J.} and D. Burt and S. Chabot and J. Ulmer and Barry, {E. M.} and Levine, {M. M.}",

note = "Funding Information: Funding: This work is supported by the European Centre for Disease Prevention and Control (ECDC); FWC No ECDC/2015/016; Specific Contract No 1 ECD.5748. Dr Manish Pareek is supported by the National Institute for Health Research (NIHR Post-Doctoral Fellowship, Dr Manish Pareek, PDF-2015-08-102). Professor Christensen acknowledges the Parker Institute, Bispebjerg and Frederiksberg Hospital and is supported by a core grant from the Oak Foundation (OCAY-13-309). The views expressed in this publication are those of the author(s) and not necessarily those of the NHS, the National Institute for Health Research or the Department of Health. Associate Professor Rachael Morton was supported by an Australian NHMRC Sidney Sax Overseas Fellowship #1054216.",

year = "2007",

month = dec,

doi = "10.1038/sj.clpt.6100420",

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Pasetti, MF, Resendiz-Albor, A, Ramirez, K, Stout, R, Papania, M, Adams, RJ, Polack, FP, Ward, BJ, Burt, D, Chabot, S, Ulmer, J, Barry, EM & Levine, MM 2007, 'Heterologous prime-boost strategy to immunize very young infants against measles: Pre-clinical studies in rhesus macaques', Clinical Pharmacology & Therapeutics, vol. 82, n.º 6, pp. 672-685. https://doi.org/10.1038/sj.clpt.6100420

TY - JOUR

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T2 - Pre-clinical studies in rhesus macaques

AU - Pasetti, M. F.

AU - Resendiz-Albor, A.

AU - Ramirez, K.

AU - Stout, R.

AU - Papania, M.

AU - Adams, R. J.

AU - Polack, F. P.

AU - Ward, B. J.

AU - Burt, D.

AU - Chabot, S.

AU - Ulmer, J.

AU - Barry, E. M.

AU - Levine, M. M.

N1 - Funding Information: Funding: This work is supported by the European Centre for Disease Prevention and Control (ECDC); FWC No ECDC/2015/016; Specific Contract No 1 ECD.5748. Dr Manish Pareek is supported by the National Institute for Health Research (NIHR Post-Doctoral Fellowship, Dr Manish Pareek, PDF-2015-08-102). Professor Christensen acknowledges the Parker Institute, Bispebjerg and Frederiksberg Hospital and is supported by a core grant from the Oak Foundation (OCAY-13-309). The views expressed in this publication are those of the author(s) and not necessarily those of the NHS, the National Institute for Health Research or the Department of Health. Associate Professor Rachael Morton was supported by an Australian NHMRC Sidney Sax Overseas Fellowship #1054216.

PY - 2007/12

Y1 - 2007/12

N2 - Infants in developing countries are at high risk of developing severe clinical measles if they become infected during the "window of vulnerability" (age 4-9 months), when declining maternal antibodies do not protect against wild virus, yet impede successful immunization by attenuated measles vaccine. We developed two Sindbis replicon-based DNA vaccines expressing measles virus hemagglutinin and fusion protein with the goal of priming young infants to respond safely and effectively to subsequent boosting with attenuated measles vaccine. Intradermal prime with DNA vaccines by needle-free injection followed by aerosol or parenteral boost with licensed measles vaccine was well tolerated by juvenile and young infant rhesus macaques, and protected against clinical measles and viremia on wild-type virus challenge. A proteosome-measles vaccine administered alone (three doses) or as a boost following DNA vaccine priming was also safe and protective. These promising results pave the way for clinical trials to assess this prime-boost strategy.

AB - Infants in developing countries are at high risk of developing severe clinical measles if they become infected during the "window of vulnerability" (age 4-9 months), when declining maternal antibodies do not protect against wild virus, yet impede successful immunization by attenuated measles vaccine. We developed two Sindbis replicon-based DNA vaccines expressing measles virus hemagglutinin and fusion protein with the goal of priming young infants to respond safely and effectively to subsequent boosting with attenuated measles vaccine. Intradermal prime with DNA vaccines by needle-free injection followed by aerosol or parenteral boost with licensed measles vaccine was well tolerated by juvenile and young infant rhesus macaques, and protected against clinical measles and viremia on wild-type virus challenge. A proteosome-measles vaccine administered alone (three doses) or as a boost following DNA vaccine priming was also safe and protective. These promising results pave the way for clinical trials to assess this prime-boost strategy.

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U2 - 10.1038/sj.clpt.6100420

DO - 10.1038/sj.clpt.6100420

M3 - Artículo

C2 - 17971812

SN - 0009-9236

VL - 82

SP - 672

EP - 685

JO - Clinical Pharmacology & Therapeutics

JF - Clinical Pharmacology & Therapeutics

IS - 6

ER -

Heterologous prime-boost strategy to immunize very young infants against measles: Pre-clinical studies in rhesus macaques

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