Abstract

Despite the widespread application of vaccination programs and antiviral drug treatments, influenza viruses are still among the most harmful human pathogens. Indeed, influenza results in significant seasonal and pandemic morbidity and mortality. Furthermore, severe bacterial infections can occur in the aftermath of influenza virus infection, and contribute substantially to the excess morbidity and mortality associated with influenza. Here, we review the main features of influenza viruses and current knowledge about the mechanical and immune mechanisms that underlie post-influenza secondary bacterial infections. We present the emerging literature describing the role of “innate-like” unconventional T cells in post-influenza bacterial superinfection. Unconventional T cell populations span the border between the innate and adaptive arms of the immune system, and are prevalent in mucosal tissues (including the airways). They mainly comprise Natural Killer T cells, mucosal-associated invariant T cells and γδ T cells. We provide an overview of the principal functions that these cells play in pulmonary barrier functions and immunity, highlighting their unique ability to sense environmental factors and promote protection against respiratory bacterial infections. We focus on two major opportunistic pathogens involved in superinfections, namely Streptococcus pneumoniae and Staphylococcus aureus. We discuss mechanisms through which influenza viruses alter the antibacterial activity of unconventional T cells. Lastly, we discuss recent fundamental advances and possible therapeutic approaches in which unconventional T cells would be targeted to prevent post-influenza bacterial superinfections.

Highlights

  • Reviewed by: Siobhan Cowley, State Food and Drug Administration, China Shilpi Chandra, La Jolla Institute for Allergy and Immunology (LJI), United States

  • Severe bacterial infections can occur in the aftermath of influenza virus infection, and contribute substantially to the excess morbidity and mortality associated with influenza

  • Before reviewing the role of “innate-like” unconventional T cells in this setting, we summarize the main mechanisms by which influenza A virus (IAV) favors secondary bacterial infection

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Summary

INFLUENZA VIRUS INFECTION AND BACTERIAL SUPERINFECTION

Respiratory infections are one the biggest health concerns worldwide. They account for a substantial rate of morbidity and mortality in Western and developing countries [1]. In general every 10 to 20 years, new influenza subtypes distinct from circulating seasonal strains can emerge (due to antigenic shift) and provoke pandemic waves with sometime devastating consequences [3]. Pandemics exhibit a higher transmissibility and a higher rate of mortality, among younger people who lack specific immunity against these new strains. During the 2009 pandemic, influenza infection had a substantial impact on human mortality [3, 6]. Severe IAV infection can lead to acute respiratory distress syndrome, a severe form of respiratory failure associated with 40 % of mortality [5]

IMMUNE RESPONSE TO IAV
RESOLUTION OF INFLAMMATION AND SECONDARY BACTERIAL INFECTION
TO SUPERINFECTION
Natural Killer T Cells
Streptococcus pneumoniae
Staphylococcus aureus
Role of Unconventional T Cells in Pulmonary Barrier Functions
Pulmonary Innate Responses
Human Studies
THERAPEUTIC OPPORTUNITIES
Findings
CONCLUSIONS AND PERSPECTIVES
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