Fatal outcome of human influenza A (H5N1) is associated with high viral load and hypercytokinemia

Jong, Menno D. de; Simmons, Cameron P.; Thanh, Tran Tan; Hien, Vo Minh; Smith, Gavin J. D.; Chau, Tran Nguyen Bich; Hoang, Dang Minh; Châu, Nguyễn Văn Vĩnh; Khanh, Truong Huu; Dong, Vo Cong; Qui, Phan Tu; Cam, Bach Van; Ha, Do Quang; Guan, Yi; Peiris, Malik; Chinh, Nguyen Tran; Hien, Tran Tinh; Farrar, Jeremy

doi:10.1038/nm1477

Cited by 1,684 publications

(1,824 citation statements)

References 28 publications

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“…Ideally, the respiratory epithelial cells should also be studied (especially for TLR3 and RLRs);3, 5, 8, 16 however, obtaining such specimens (e.g., with bronchoalveolar lavage ) is generally infeasible in patients with influenza. Studying circulating cells exposed to the pulmonary bed has been shown to provide close estimates 6, 7, 20, 22, 32, 41. Although the inclusion of a “mild influenza” group might be helpful, earlier studies have indicated that inflammatory cytokine responses are barely detectable in such patients 20, 22, 27.…”

Section: Discussionmentioning

confidence: 99%

Role of human Toll‐like receptors in naturally occurring influenza A infections

Lee

Wong

Hui

et al. 2013

Influenza Resp Viruses

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BackgroundWe investigated the roles of Toll‐like receptors (TLRs) in naturally occurring influenza.MethodsA prospective, case – control study was conducted. Adults hospitalized with virologically confirmed influenza A infections (onset <48 hours, before treatment) were compared with age‐/gender‐matched controls. TLRs (2, 3, 4, 7, 8, 9) expression in monocytes and dendritic cells (DCs – total, myeloid, plasmacytoid) was quantitated using flow cytometry. Gene expression of RLRs (RIG‐1, MDA‐5) was evaluated using real‐time PCR. Concomitant signaling molecules expression, plasma cytokine/chemokine concentrations, and respiratory tract viral loads were measured. PBMCs were cultured and stimulated ex vivo with TLR‐specific ligands for cytokine responses.ResultsForty two patients with influenza (24 A/H3N2, 18 A/H1N1pdm09) and 20 controls were studied. Patients' mean age was 68 ± 16 years; 81% had respiratory/cardiovascular complications. There were increased cellular expressions of TLR9, TLR8, TLR3, and TLR7 during influenza; TLR2 and TLR4 were suppressed. Results were similar for both virus strains. Higher TLR expression levels at presentation significantly correlated with lower viral loads (Spearman's rho: −0·46 to −0·69 for TLR9, TLR8, and TLR3; P‐values <0·05). Multivariate regression models (adjusted for age, comorbidity, disease severity, time from onset) confirmed their independent associations. Increased signaling molecules (phospho‐MAPKs, IκB) and inflammatory cytokines (IL‐6, sTNFR‐1, CCL2/MCP‐1; CXCL10/IP‐10, IFN‐γ) correlated with increased TLR expression. RLRs were upregulated simultaneously. PBMCs of patients with influenza showed significant, dynamic changes in their cytokine responses upon TLR stimulation, compared with controls.ConclusionsOur results suggest that TLRs play an important role in early, innate viral inhibition in naturally occurring influenza. Inflammatory cytokine responses are concomitantly induced. These findings support investigation of TLR targeting as a novel intervention approach for prophylaxis against influenza.

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Section: Discussionmentioning

confidence: 99%

Role of human Toll‐like receptors in naturally occurring influenza A infections

Lee

Wong

Hui

et al. 2013

Influenza Resp Viruses

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“…Subjects were participants in a large prospective study of rapid near patient testing for Streptococcus pneumoniae and influenza and met the following inclusion criteria; adult aged over 18 years of age, able and willing to give written informed consent (or a relative or carer is able and willing to give informed assent), acute exacerbation of a chronic respiratory disease or new onset of acute respiratory illness, of less than 7 days duration, able to be recruited within 16 Patients were tested for respiratory virus infection as detailed below and those testing positive for respiratory viruses and with viral load data available were included in this study. Patients with dual viral detections were excluded.…”

Section: Patientsmentioning

confidence: 99%

“…In hospitalised patients with the virulent avian H5N1 influenza A, who generally have life threatening disease, the pharyngeal viral load on admission to hospital is higher than in patients with seasonal influenza [16] and is higher in non-survivors versus those who survive [17].…”

Section: Introductionmentioning

confidence: 99%

Viral load is strongly associated with length of stay in adults hospitalised with viral acute respiratory illness

Clark

Ewings

Medina

et al. 2016

Journal of Infection

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“…For example, type I interferons have strong antiviral activities and can directly inhibit influenza virus replication 1, 2. Meanwhile, excessive cytokine/chemokine responses have been associated with more severe disease during the 2009 H1N1 pandemic,3 lung damage in macaques infected with the 1918 influenza virus,4 and fatal H5N1 infection in humans 5…”

Section: Introductionmentioning

confidence: 99%

Rapid changes in serum cytokines and chemokines in response to inactivated influenza vaccination

Talaat

Halsey

Cox

et al. 2018

Influenza Resp Viruses

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BackgroundThe timing of host cytokine responses to influenza vaccination is poorly understood.ObjectivesWe examined serum cytokine kinetics following inactivated trivalent influenza vaccine (TIV) to better understand potential relationships between markers of inflammation and TIV‐related side effects.Patients/MethodsTwenty healthy adult subjects received TIV. Cytokines/chemokines were assessed in intervals from 3 hours to 14 days. Antibody titers were measured at baseline and Day 14.ResultsSerum cytokine responses to TIV were evident as early as 3 hours post‐immunization. Compared to baseline, IFN‐γ and IP‐10 were significantly elevated 7 hours after TIV administration. Both remained elevated and peaked between 16 and 24 hours before returning to baseline by 44 hours post‐vaccination. Although IL‐8 levels were variable between subjects during the first 24 hours after TIV, by 44 hours, IL‐8 was significantly lower compared to baseline. Interestingly, IL‐8 levels remained significantly lower for up to 2 weeks after receiving TIV. Fifteen of 20 subjects reported mild adverse events. The one subject who reported moderate myalgias and injection site pain after vaccination displayed a distinctive, early cytokine response profile which included IL‐6, IL‐2, IL‐8, IP‐10, MCP‐1, TNF‐α, TARC, and MCP‐4.ConclusionsSerum cytokines changed rapidly following TIV and generally peaked at 24 hours. Trivalent influenza vaccine‐induced reductions in IL‐8 occurred later (44 hours) and were sustained for 2 weeks. An outlier response coincided with the only moderate side effects to the vaccine. These data suggest that early cytokine/chemokine responses may provide additional insight into the pathogenesis of adverse events and immune reactivity to vaccination.

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Fatal outcome of human influenza A (H5N1) is associated with high viral load and hypercytokinemia

Cited by 1,684 publications

References 28 publications

Role of human Toll‐like receptors in naturally occurring influenza A infections

Role of human Toll‐like receptors in naturally occurring influenza A infections

Viral load is strongly associated with length of stay in adults hospitalised with viral acute respiratory illness

Rapid changes in serum cytokines and chemokines in response to inactivated influenza vaccination

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