Potent protection against H5N1 and H7N9 influenza via childhood hemagglutinin imprinting

Gostic, Katelyn M.; Ambrose, Monique; Worobey, Michael; Lloyd‐Smith, James O.

doi:10.1126/science.aag1322

Cited by 398 publications

(393 citation statements)

References 64 publications

(78 reference statements)

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“…In recent years, avian influenza virus H5N1 and H7N9 subtypes have caused hundreds of human infections with a mortality rate of 20% to 60% [9]. Studies have demonstrated that “original antigenic sin” [138] is a key determinant for the susceptibility of zoonotic influenza viruses [138–140]. “Original antigenic sin” arises when our immune system employs immunological memory based on an earlier infection by a virus with an slightly different antigenicity, which then skews the current immune response towards antibodies that were previously produced and to epitopes recognized during previous infections [138].…”

Section: Protective Immunity Against Zoonotic Influenza Virusesmentioning

confidence: 99%

“…Based on statistical modeling, such childhood imprinting is also important for determining the susceptibility against emerging avian influenza viruses H5N1 and H7N9 subtypes [140]. Briefly, those who were infected with seasonal H1 or H2 subtype (group 1) during their first encounter of influenza virus are less susceptible to H5 viruses (group 1), whereas those who were infected with seasonal H3 subtype (group 2) during their first encounter of influenza virus are less susceptible to H7 viruses (group 2) [140]. Overall, these observations highlight the importance of “original antigenic sin” in protection against zoonotic influenza viruses.…”

Section: Protective Immunity Against Zoonotic Influenza Virusesmentioning

confidence: 99%

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A Perspective on the Structural and Functional Constraints for Immune Evasion: Insights from Influenza Virus

Wilson

2017

Journal of Molecular Biology

142

174

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Influenza virus evolves rapidly to constantly escape from natural immunity. Most humoral immune responses to influenza virus target the hemagglutinin glycoprotein (HA), which is the major antigen on the surface of the virus. The HA is comprised of a globular head domain for receptor binding and a stem domain for membrane fusion. The major antigenic sites of HA are located in the globular head subdomain, which is highly tolerant of amino-acid substitutions and continual addition of glycosylation sites. Nonetheless, the evolution of the receptor-binding site (RBS) and the stem region on HA is severely constrained by their functional roles in engaging the host receptor and in mediating membrane fusion, respectively. Here, we review how broadly neutralizing antibodies (bnAbs) exploit these evolutionary constraints to protect against diverse influenza strains. We also discuss the emerging role of other epitopes that are conserved only in subsets of viruses. This rapidly increasing knowledge of the evolutionary biology, immunology, structural biology, and virology of influenza virus is invaluable for development and design of more universal influenza vaccines as well as novel therapeutics.

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Section: Protective Immunity Against Zoonotic Influenza Virusesmentioning

confidence: 99%

Section: Protective Immunity Against Zoonotic Influenza Virusesmentioning

confidence: 99%

A Perspective on the Structural and Functional Constraints for Immune Evasion: Insights from Influenza Virus

Wilson

2017

Journal of Molecular Biology

142

174

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“…Such Th17 memory responses may help protect the lungs against serotypes of pneumococcus that are not in vaccines or the previous experience of that individual. In humans, immunological “imprinting” from first influenza infections in childhood was observed to help prevent severe pneumonia from multiple sub-types within that phylogenetic group but not from other phylogenetic groups (e.g., H1 infections are good for later infections with H2 or H5 but not H3 or H7, whereas H3 is good against subsequent H7 but not H1, H2, or H5 infections) (22). Such heterotypic protection that results from first infections may explain some of the variations across differently aged cohorts to severe infections from different strains of influenza.…”

Section: Advances In Immune Resistancementioning

confidence: 99%

Pathogenesis of severe pneumonia

Mizgerd

2017

Current Opinion in Pulmonary Medicine

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Purpose of review Pneumonia is a common disease that becomes severe in a subset of patients, dependent on host biology including mechanisms of immune resistance and tissue resilience. This review emphasizes discoveries in pneumonia biology from 2016, highlighting questions and directions that are especially pressing or newly emerging. Recent findings Novel cell-cell interactions mediating innate immune responses against microbes in the lung have been elucidated, between distinct leukocyte sub-types as well as between leukocytes and the structural cells of the lung. Adaptive immunity has received growing attention for determining the outcome of pneumonia, particularly the lung resident memory cells that arise from repeated prior respiratory infections and direct heterotypic recall responses. New tissue resilience components have been identified that contribute to anti-inflammatory, pro-resolution, tissue-protective, and reparative regeneration pathways in the infected lung. Summary Recent findings will direct research into fundamental mechanisms of lung protection. Over the longer term, manipulating these pathways has implications for clinical practice, as strategies to bolster resistance and resilience have potential to ameliorate severe pneumonia.

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“…Pneumonia defense is strongly influenced by the earliest infections with respiratory pathogens, based on evidence of immunological "imprinting" against influenza viruses (167). Those born before 1968 were likely first infected with influenza viruses containing hemagglutinins (HAs) from phylogenetic group 1 (which includes H1, H2, and H5 HAs), whereas those born after that date were more likely to be first infected by influenza viruses with group 2 HAs (which includes H3 and H7 HAs).…”

Section: A Naturally Acquired Heterotypic Adaptive Immunitymentioning

confidence: 99%

Integrative Physiology of Pneumonia

Quinton

Walkey

Mizgerd

2018

Physiological Reviews

189

203

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Pneumonia is a type of acute lower respiratory infection that is common and severe. The outcome of lower respiratory infection is determined by the degrees to which immunity is protective and inflammation is damaging. Intercellular and interorgan signaling networks coordinate these actions to fight infection and protect the tissue. Cells residing in the lung initiate and steer these responses, with additional immunity effectors recruited from the bloodstream. Responses of extrapulmonary tissues, including the liver, bone marrow, and others, are essential to resistance and resilience. Responses in the lung and extrapulmonary organs can also be counterproductive and drive acute and chronic comorbidities after respiratory infection. This review discusses cell-specific and organ-specific roles in the integrated physiological response to acute lung infection, and the mechanisms by which intercellular and interorgan signaling contribute to host defense and healthy respiratory physiology or to acute lung injury, chronic pulmonary disease, and adverse extrapulmonary sequelae. Pneumonia should no longer be perceived as simply an acute infection of the lung. Pneumonia susceptibility reflects ongoing and poorly understood chronic conditions, and pneumonia results in diverse and often persistent deleterious consequences for multiple physiological systems.

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Potent protection against H5N1 and H7N9 influenza via childhood hemagglutinin imprinting

Cited by 398 publications

References 64 publications

A Perspective on the Structural and Functional Constraints for Immune Evasion: Insights from Influenza Virus

A Perspective on the Structural and Functional Constraints for Immune Evasion: Insights from Influenza Virus

Pathogenesis of severe pneumonia

Integrative Physiology of Pneumonia

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