Early hypercytokinemia is associated with interferon-induced transmembrane protein-3 dysfunction and predictive of fatal H7N9 infection

Zhongfang Wang(Shanghai Medical College of Fudan University), Anli Zhang(Shanghai Medical College of Fudan University), Yanmin Wan(Shanghai Medical College of Fudan University), Xinian Liu(Shanghai Medical College of Fudan University), Chao Qiu(Shanghai Medical College of Fudan University), Xiuhong Xi(Shanghai Medical College of Fudan University), Yanqin Ren(Shanghai Medical College of Fudan University), Jing Wang(Shanghai Medical College of Fudan University), Yuan Dong(Shanghai Medical College of Fudan University), Meijuan Bao(Shanghai Medical College of Fudan University), Liangzhu Li(Shanghai Medical College of Fudan University), Mingzhe Zhou(Shanghai Medical College of Fudan University), Songhua Yuan(Shanghai Medical College of Fudan University), Jun Sun(Shanghai Medical College of Fudan University), Zhaoqin Zhu(Shanghai Medical College of Fudan University), Liang Chen(Shanghai Medical College of Fudan University), Qingsheng Li(University of Nebraska–Lincoln), Zhiyong Zhang(Shanghai Medical College of Fudan University), Xiaoyan Zhang(Centers for Disease Control and Prevention), Shuihua Lu(Shanghai Medical College of Fudan University), Peter C. Doherty(St. Jude Children's Research Hospital), Katherine Kedzierska(The University of Melbourne), Jianqing Xu(Centers for Disease Control and Prevention)
Proceedings of the National Academy of Sciences
December 23, 2013
Cited by 287Open Access
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Abstract

A unique avian-origin A/H7N9 influenza virus has so far caused 134 cases with 44 deaths. Probing the host factors contributing to disease severity, we found that lower levels of plasma inflammatory cytokines on hospital admission correlated with faster recovery in 18 patients with A/H7N9 influenza virus, whereas high concentrations of (in particular) IL-6, IL-8, and macrophage inflammatory protein-1β were predictive of a less favorable or fatal outcome. Analysis of bronchoalveolar lavage samples showed up to 1,000-fold greater cytokine/chemokine levels relative to plasma. Furthermore, patients with the rs12252-C/C IFN-induced transmembrane protein-3 (IFITM3) genotype had more rapid disease progression and were less likely to survive. Compared with patients with the rs12252-T/T or rs12252-T/C genotype of IFITM3, patients with the C/C genotype had a shorter time from disease onset to the time point when they sought medical aid (hospital admission or antiviral therapy) and a shorter interval to development of the acute respiratory distress syndrome stage (reflected by shorter intervals between clinical onset and methylprednisolone treatments and higher rates of mechanical ventilator use), as well as experiencing elevated/prolonged lung virus titers and cytokine production and higher mortality. The present analysis provides reported data on the H7N9 influenza-induced "cytokine storm" at the site of infection in humans and identifies the rs12252-C genotype that compromises IFITM3 function as a primary genetic correlate of severe H7N9 pneumonia. Together with rs12252 sequencing, early monitoring of plasma cytokines is thus of prognostic value for the treatment and management of severe influenza pneumonia.


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