Tropism and Innate Host Responses of the 2009 Pandemic H1N1 Influenza Virus in ex Vivo and in Vitro Cultures of Human Conjunctiva and Respiratory Tract

Chan, Michael Chi Wai; Chan, Renee W. Y.; Yu, Wai Cho; Ho, Carol C. C.; Yuen, Kit M.; Fong, Joanne H. M.; Tang, Lynsia Ls; Lai, Wico W.; Lo, Amy Cheuk Yin; Chui, Wing Hung; Sihoe, Alan D. L.; Kwong, Dora Lai-Wan; Wong, David; Tsao, George S.W.; Poon, Leo L. M.; Guan, Yi; Nicholls, John M.; Peiris, J. S. Malik

doi:10.2353/ajpath.2010.091087

Cited by 112 publications

(150 citation statements)

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“…Of interest, a number of studies have established that seasonal and pandemic H1N1 viruses elicit similar innate responses from human airway cells. Seasonal and pandemic H1N1 viruses were both poor in their ability to induce expression of antiviral and inflammatory cytokine genes from human dendritic cells and macrophages (45), and did not differ in ability to induce proinflammatory cytokines from human pneumocytes and bronchiolar epithelial cells (46). Recognition of sialylated residues on NKp46 by the HA of seasonal or pandemic H1N1 viruses also induced NK cell-mediated killing of virusinfected target cells (47).…”

Section: Discussionmentioning

confidence: 99%

“…Initial studies demonstrated preferential binding of A(H1N1) pdm viruses to a2,6-linked sialic acids (11) although subsequent glycan array data indicate significant binding to both a2,6-linked and a2,3-linked sialic acids, unlike seasonal H1N1 viruses that showed a distinct preference for a2,6-linked sialic acids (48). Seasonal H1N1, H3N2, and A(H1N1) pdm viruses replicated to comparable levels in ex vivo cultures of human nasopharynx and lung tissues, but human conjunctiva showed preferential susceptibility to infection by A(H1N1) pdm (46), consistent with subtle differences in receptor specificity that could potentially affect pathogenesis in humans.…”

Section: Discussionmentioning

confidence: 99%

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Pandemic H1N1 Influenza A Viruses Are Resistant to the Antiviral Activities of Innate Immune Proteins of the Collectin and Pentraxin Superfamilies

Job

Deng

Tate

et al. 2010

The Journal of Immunology

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Acquired immune responses elicited to recent strains of seasonal H1N1 influenza viruses provide limited protection against emerging A(H1N1) pandemic viruses. Accordingly, pre-existing or rapidly induced innate immune defenses are of critical importance in limiting early infection. Respiratory secretions contain proteins of the innate immune system, including members of the collectin and pentraxin superfamilies. These mediate potent antiviral activity and act as an initial barrier to influenza infection. In this study, we have examined the sensitivity of H1N1 viruses, including pandemic virus strains, for their sensitivity to collectins (surfactant protein [SP]-D and mannose-binding lectin [MBL]) and to the pentraxin PTX3. Human SP-D and MBL inhibited virus-induced hemagglutinating activity, blocked the enzymatic activity of the viral neuraminidase, and neutralized the ability of H1N1 viruses to infect human respiratory epithelial cells in a manner that correlated with the degree of glycosylation in the globular head of the hemagglutinin. Recent seasonal H1N1 viruses expressed three to four N-glycosylation sequons on the head of hemagglutinin and were very sensitive to inhibition by SP-D or MBL, whereas A(H1N1) pandemic viruses expressed a single N-glycosylation sequon and were resistant to either collectin. Of interest, both seasonal and pandemic H1N1 viruses were resistant to PTX3. Thus, unlike recent seasonal H1N1 strains of influenza virus, A(H1N1) pandemic viruses are resistant to the antiviral activities of innate immune proteins of the collectin superfamily.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Pandemic H1N1 Influenza A Viruses Are Resistant to the Antiviral Activities of Innate Immune Proteins of the Collectin and Pentraxin Superfamilies

Job

Deng

Tate

et al. 2010

The Journal of Immunology

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“…Currently there are mixed conclusions reported regarding what cell type is preferred by seasonal IAV with data supporting binding to ciliated and/or non-ciliated (goblet) cells [61,66]. Seasonal and H1N1pdm IAVs enter and replicate efficiently in ciliated cells that line the epithelial cell layer in the large and small airways of the respiratory tract, while H5N1 enters and replicates more efficiently in non-ciliated cells (type II pneumocytes) within the small lower airways ( Figure 3B) [74,75,[83][84][85][86][87].…”

Section: Influenza a Virus Life Cycyle Attachment And Bindingmentioning

confidence: 99%

“…Moreover a large percentage of children without pre-existing comorbidities presented with upper and lower respiratory tract involvement. This led some researchers in the influenza field to ask whether the HA had a broader specificity for human receptors since the HA of this virus had an avian origin [66, [74][75][76]. One avian signature of the HA is at the G position 222 in the HA [77,78].…”

Section: Influenza a Virus Life Cycyle Attachment And Bindingmentioning

confidence: 99%

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Early host response and immune signaling to 2009 pandemic influenza A (H1N1) viruses in primary cell culture models.

Gerlach¹

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The 2009 Pandemic Influenza Virus: Where Did It Come from, Where Is It Now, and Where Is It Going?

York

Donis

2012

Swine Influenza

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Around 2008 or 2009, an influenza A virus that had been circulating undetected in swine entered human population. Unlike most swine influenza infections of humans, this virus established sustained human-to-human transmission, leading to a global pandemic. The virus responsible, 2009 pandemic H1N1 (H1N1pdm), is the result of multiple reassortment events that brought together genomic segments from classical H1N1 swine influenza virus, human seasonal H3N2 influenza virus, North American avian influenza virus, and Eurasian avian-origin swine influenza viruses. Genetically, H1N1pdm possesses a number of unusual features, although the genomic characteristics that permitted sustained human-to-human transmission are yet unclear. Human infection with H1N1pdm has generally resulted in low mortality, although certain subgroups (including pregnant women, people with some chronic medical conditions, morbidly obese individuals, and immunosuppressed people) have significantly higher risk of severe disease. As H1N1pdm has spread throughout the human population it continued to evolve. It has also reentered the swine population as a circulating pathogen, and has been transiently identified in other species such as turkeys, cats, and domestic ferrets. Most genetic changes in H1N1pdm to date have not been clearly linked to changes in antigenicity, disease severity, antiviral drug resistance, or transmission efficiency. However, the rapid evolution rate characteristic of influenza viruses suggests that changes in antigenicity are inevitable in future years. Experience with this first pandemic of twenty-first century reemphasizes the importance of influenza surveillance in animals as well as humans, and offers lessons to develop and enhance our ability to identify potentially pandemic influenza viruses in the future.

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Tropism and Innate Host Responses of the 2009 Pandemic H1N1 Influenza Virus in ex Vivo and in Vitro Cultures of Human Conjunctiva and Respiratory Tract

Cited by 112 publications

References 27 publications

Pandemic H1N1 Influenza A Viruses Are Resistant to the Antiviral Activities of Innate Immune Proteins of the Collectin and Pentraxin Superfamilies

Pandemic H1N1 Influenza A Viruses Are Resistant to the Antiviral Activities of Innate Immune Proteins of the Collectin and Pentraxin Superfamilies

Early host response and immune signaling to 2009 pandemic influenza A (H1N1) viruses in primary cell culture models.

The 2009 Pandemic Influenza Virus: Where Did It Come from, Where Is It Now, and Where Is It Going?

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