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Sensing prokaryotic mRNA signifies microbial viability and promotes immunity

Live vaccines have long been known to trigger far more vigorous immune responses than their killed counterparts(1–6). This has been attributed to the ability of live microorganisms to replicate and express specialized virulence factors that facilitate invasion and infection of their hosts(7). Howeve...

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Autores principales: Sander, Leif E., Davis, Michael J., Boekschoten, Mark V., Amsen, Derk, Dascher, Christopher C., Ryffel, Bernard, Swanson, Joel A., Müller, Michael, Blander, J. Magarian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3289942/
https://www.ncbi.nlm.nih.gov/pubmed/21602824
http://dx.doi.org/10.1038/nature10072
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author Sander, Leif E.
Davis, Michael J.
Boekschoten, Mark V.
Amsen, Derk
Dascher, Christopher C.
Ryffel, Bernard
Swanson, Joel A.
Müller, Michael
Blander, J. Magarian
author_facet Sander, Leif E.
Davis, Michael J.
Boekschoten, Mark V.
Amsen, Derk
Dascher, Christopher C.
Ryffel, Bernard
Swanson, Joel A.
Müller, Michael
Blander, J. Magarian
author_sort Sander, Leif E.
collection PubMed
description Live vaccines have long been known to trigger far more vigorous immune responses than their killed counterparts(1–6). This has been attributed to the ability of live microorganisms to replicate and express specialized virulence factors that facilitate invasion and infection of their hosts(7). However, protective immunization can often be achieved with a single injection of live, but not dead, attenuated microorganisms stripped of their virulence factors. Pathogen associated molecular patterns (PAMPs), which serve to alert the immune system(8,9), are present in both live and killed vaccines, suggesting that certain poorly characterized aspects of live microorganisms, not incorporated in dead vaccines, are particularly effective at inducing protective immunity. Here we show that the innate immune system can directly sense microbial viability through detection of a special class of viability-associated PAMPs (vita-PAMPs). We identify prokaryotic messenger RNA (mRNA) as a vita-PAMP present only in viable bacteria, recognition of which elicits a unique innate response and a robust adaptive antibody response. Notably, the innate response evoked by viability and prokaryotic mRNA was thus far considered to be reserved for pathogenic bacteria, but we show that even nonpathogenic bacteria in sterile tissues can trigger similar responses, provided they are alive. Thus, the immune system actively gauges the infectious risk by scouring PAMPs for signatures of microbial life and thus infectivity. Detection of vita-PAMPs triggers an alert mode not warranted for dead bacteria. Vaccine formulations that incorporate vita-PAMPs could thus combine the superior protection of live vaccines with the safety of dead vaccines.
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spelling pubmed-32899422012-02-29 Sensing prokaryotic mRNA signifies microbial viability and promotes immunity Sander, Leif E. Davis, Michael J. Boekschoten, Mark V. Amsen, Derk Dascher, Christopher C. Ryffel, Bernard Swanson, Joel A. Müller, Michael Blander, J. Magarian Nature Article Live vaccines have long been known to trigger far more vigorous immune responses than their killed counterparts(1–6). This has been attributed to the ability of live microorganisms to replicate and express specialized virulence factors that facilitate invasion and infection of their hosts(7). However, protective immunization can often be achieved with a single injection of live, but not dead, attenuated microorganisms stripped of their virulence factors. Pathogen associated molecular patterns (PAMPs), which serve to alert the immune system(8,9), are present in both live and killed vaccines, suggesting that certain poorly characterized aspects of live microorganisms, not incorporated in dead vaccines, are particularly effective at inducing protective immunity. Here we show that the innate immune system can directly sense microbial viability through detection of a special class of viability-associated PAMPs (vita-PAMPs). We identify prokaryotic messenger RNA (mRNA) as a vita-PAMP present only in viable bacteria, recognition of which elicits a unique innate response and a robust adaptive antibody response. Notably, the innate response evoked by viability and prokaryotic mRNA was thus far considered to be reserved for pathogenic bacteria, but we show that even nonpathogenic bacteria in sterile tissues can trigger similar responses, provided they are alive. Thus, the immune system actively gauges the infectious risk by scouring PAMPs for signatures of microbial life and thus infectivity. Detection of vita-PAMPs triggers an alert mode not warranted for dead bacteria. Vaccine formulations that incorporate vita-PAMPs could thus combine the superior protection of live vaccines with the safety of dead vaccines. 2011-05-22 /pmc/articles/PMC3289942/ /pubmed/21602824 http://dx.doi.org/10.1038/nature10072 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Sander, Leif E.
Davis, Michael J.
Boekschoten, Mark V.
Amsen, Derk
Dascher, Christopher C.
Ryffel, Bernard
Swanson, Joel A.
Müller, Michael
Blander, J. Magarian
Sensing prokaryotic mRNA signifies microbial viability and promotes immunity
title Sensing prokaryotic mRNA signifies microbial viability and promotes immunity
title_full Sensing prokaryotic mRNA signifies microbial viability and promotes immunity
title_fullStr Sensing prokaryotic mRNA signifies microbial viability and promotes immunity
title_full_unstemmed Sensing prokaryotic mRNA signifies microbial viability and promotes immunity
title_short Sensing prokaryotic mRNA signifies microbial viability and promotes immunity
title_sort sensing prokaryotic mrna signifies microbial viability and promotes immunity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3289942/
https://www.ncbi.nlm.nih.gov/pubmed/21602824
http://dx.doi.org/10.1038/nature10072
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