Direct association between pharyngeal viral secretion and host cytokine response in severe pandemic influenza

Raquel Almansa,Ana Loza,David Andaluz,Longsi Ran,Luoling Xu,Salvador Resino,Felipe Bobillo,Paula Mateo,Pedro Merino,Jordi Rello,Francisco Gandía,Carmen Castro,Tomás Pumarola ,Raúl Ortíz De Lejarazu ,José M Eiros ,E Maraví ,Paula Ramírez ,Mónica Gordon ,Milagros González-Rivera ,Lorenzo Socías ,David J Kelvin ,Victoria Fernández ,Guillermo López–Campos ,Fernando Martín-Sánchez ,David W Banner ,Maria C Gallegos,Jesús Blanco,María Ángeles Marcos ,Andrés Antón ,Cristóbal León ,Ignacio Martín‐Loeches ,Jesús F Bermejo‐Martin

doi:10.1186/1471-2334-11-232

Abstract

BackgroundSevere disease caused by 2009 pandemic influenza A/H1N1virus is characterized by the presence of hypercytokinemia. The origin of the exacerbated cytokine response is unclear. As observed previously, uncontrolled influenza virus replication could strongly influence cytokine production. The objective of the present study was to evaluate the relationship between host cytokine responses and viral levels in pandemic influenza critically ill patients.MethodsTwenty three patients admitted to the ICU with primary viral pneumonia were included in this study. A quantitative PCR based method targeting the M1 influenza gene was developed to quantify pharyngeal viral load. In addition, by using a multiplex based assay, we systematically evaluated host cytokine responses to the viral infection at admission to the ICU. Correlation studies between cytokine levels and viral load were done by calculating the Spearman correlation coefficient.ResultsFifteen patients needed of intubation and ventilation, while eight did not need of mechanical ventilation during ICU hospitalization. Viral load in pharyngeal swabs was 300 fold higher in the group of patients with the worst respiratory condition at admission to the ICU. Pharyngeal viral load directly correlated with plasma levels of the pro-inflammatory cytokines IL-6, IL-12p70, IFN-γ, the chemotactic factors MIP-1β, GM-CSF, the angiogenic mediator VEGF and also of the immuno-modulatory cytokine IL-1ra (p < 0.05). Correlation studies demonstrated also the existence of a significant positive association between the levels of these mediators, evidencing that they are simultaneously regulated in response to the virus.ConclusionsSevere respiratory disease caused by the 2009 pandemic influenza virus is characterized by the existence of a direct association between viral replication and host cytokine response, revealing a potential pathogenic link with the severe disease caused by other influenza subtypes such as H5N1.

Highlights

Severe disease caused by 2009 pandemic influenza A/H1N1virus is characterized by the presence of hypercytokinemia
The objective of the present study was to evaluate the relationship between host cytokine responses and pharyngeal viral load in pandemic influenza critically ill patients at admission to the ICU
Patients were admitted to ICU five days in average following the onset of the symptoms

Summary

Introduction

Severe disease caused by 2009 pandemic influenza A/H1N1virus is characterized by the presence of hypercytokinemia. As observed previously, uncontrolled influenza virus replication could strongly influence cytokine production. The objective of the present study was to evaluate the relationship between host cytokine responses and viral levels in pandemic influenza critically ill patients. Severe obesity, cardiovascular disease and diabetes have been reported as risk factors for critical illness following infection with the pandemic virus [1,2]. A exacerbated cytokine response can contribute to immunemediated tissue damage during viral infections [9,10]. In this sense, unregulated cytokine and interferon responses have been described to parallel persistence of viral replication and severe disease in SARS [11]. As previously described, uncontrolled influenza virus replication could strongly influence cytokine production [5,12,13]

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