Th1 and Th17 hypercytokinemia as early host response signature in severe pandemic influenza

Human host immune response following infection with the new variant of A/H1N1 pandemic influenza virus (nvH1N1) is poorly understood. We utilize here systemic cytokine and antibody levels in evaluating differences in early immune response in both mild and severe patients infected with nvH1N1. We pro...

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Bibliographic Details
Published in:Critical care (London, England) England), 2009-01, Vol.13 (6), p.R201-R201, Article R201
Main Authors: Bermejo-Martin, Jesus F, Ortiz de Lejarazu, Raul, Pumarola, Tomas, Rello, Jordi, Almansa, Raquel, Ramírez, Paula, Martin-Loeches, Ignacio, Varillas, David, Gallegos, Maria C, Serón, Carlos, Micheloud, Dariela, Gomez, Jose Manuel, Tenorio-Abreu, Alberto, Ramos, María J, Molina, M Lourdes, Huidobro, Samantha, Sanchez, Elia, Gordón, Mónica, Fernández, Victoria, Del Castillo, Alberto, Marcos, Ma Angeles, Villanueva, Beatriz, López, Carlos Javier, Rodríguez-Domínguez, Mario, Galan, Juan-Carlos, Cantón, Rafael, Lietor, Aurora, Rojo, Silvia, Eiros, Jose M, Hinojosa, Carmen, Gonzalez, Isabel, Torner, Nuria, Banner, David, Leon, Alberto, Cuesta, Pablo, Rowe, Thomas, Kelvin, David J
Format: Article
Language:English
Subjects:
Adult
Analysis
Chemokines - blood
Complications and side effects
Cytokines
Cytokines - blood
Development and progression
DNA Primers
Female
Health aspects
Hemagglutination Inhibition Tests
Humans
Immune response
Influenza A Virus, H1N1 Subtype - genetics
Influenza, Human - blood
Influenza, Human - pathology
Influenza, Human - physiopathology
Intensive Care Units
Length of Stay
Male
Middle Aged
Patient Selection
RNA, Viral - isolation & purification
Severity of Illness Index
Swine influenza
Th1 Cells - physiology
Viral Load
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Summary:Human host immune response following infection with the new variant of A/H1N1 pandemic influenza virus (nvH1N1) is poorly understood. We utilize here systemic cytokine and antibody levels in evaluating differences in early immune response in both mild and severe patients infected with nvH1N1. We profiled 29 cytokines and chemokines and evaluated the haemagglutination inhibition activity as quantitative and qualitative measurements of host immune responses in serum obtained during the first five days after symptoms onset, in two cohorts of nvH1N1 infected patients. Severe patients required hospitalization (n = 20), due to respiratory insufficiency (10 of them were admitted to the intensive care unit), while mild patients had exclusively flu-like symptoms (n = 15). A group of healthy donors was included as control (n = 15). Differences in levels of mediators between groups were assessed by using the non parametric U-Mann Whitney test. Association between variables was determined by calculating the Spearman correlation coefficient. Viral load was performed in serum by using real-time PCR targeting the neuraminidase gene. Increased levels of innate-immunity mediators (IP-10, MCP-1, MIP-1beta), and the absence of anti-nvH1N1 antibodies, characterized the early response to nvH1N1 infection in both hospitalized and mild patients. High systemic levels of type-II interferon (IFN-gamma) and also of a group of mediators involved in the development of T-helper 17 (IL-8, IL-9, IL-17, IL-6) and T-helper 1 (TNF-alpha, IL-15, IL-12p70) responses were exclusively found in hospitalized patients. IL-15, IL-12p70, IL-6 constituted a hallmark of critical illness in our study. A significant inverse association was found between IL-6, IL-8 and PaO2 in critical patients. While infection with the nvH1N1 induces a typical innate response in both mild and severe patients, severe disease with respiratory involvement is characterized by early secretion of Th17 and Th1 cytokines usually associated with cell mediated immunity but also commonly linked to the pathogenesis of autoimmune/inflammatory diseases. The exact role of Th1 and Th17 mediators in the evolution of nvH1N1 mild and severe disease merits further investigation as to the detrimental or beneficial role these cytokines play in severe illness.
ISSN:1364-8535
1466-609X
1364-8535
DOI:10.1186/cc8208