Rhinovirus-induced lower respiratory illness is increased in asthma and related to virus load and Th1/2 cytokine and IL-10 production

Message, Simon D.; Laza-Stanca, Vasile; Mallia, Patrick; Parker, Hayley L.; Zhu, Jie; Kebadze, Tatiana; Contoli, Marco; Sanderson, G.; Kon, Onn Min; Papi, Alberto; Jeffery, Peter K.; Stanciu, Luminita A.; Johnston, Sebastian L.

doi:10.1073/pnas.0804181105

Cited by 451 publications

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“…18,19 Viral infection impairs antibacterial innate immune responses 20 and increases bacterial adherence to bronchial epithelium. 21 Thus, bacterial infections are more common and more severe in patients with asthma, viruses increase susceptibility to bacterial infection, and acute wheezing episodes in children younger than 3 years were associated with both bacterial and viral infection.…”

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confidence: 99%

Azithromycin for Acute Exacerbations of Asthma

et al. 2016

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IMPORTANCEGuidelines recommend against antibiotic use to treat asthma attacks. A study with telithromycin reported benefit, but adverse reactions limit its use.OBJECTIVE To determine whether azithromycin added to standard care for asthma attacks in adults results in clinical benefit. DESIGN, SETTING, AND PARTICIPANTSThe Azithromycin Against Placebo in Exacerbations of Asthma (AZALEA) randomized, double-blind, placebo-controlled clinical trial, a United Kingdom-based multicenter study in adults requesting emergency care for acute asthma exacerbations, ran from September 2011 to April 2014. Adults with a history of asthma for more than 6 months were recruited within 48 hours of presentation to medical care with an acute deterioration in asthma control requiring a course of oral and/or systemic corticosteroids.INTERVENTIONS Azithromycin 500 mg daily or matched placebo for 3 days. MAIN OUTCOMES AND MEASURESThe primary outcome was diary card symptom score 10 days after randomization, with a hypothesized treatment effect size of −0.3. Secondary outcomes were diary card symptom score, quality-of-life questionnaires, and lung function changes, all between exacerbation and day 10, and time to a 50% reduction in symptom score. RESULTSOf 4582 patients screened at 31 centers, 199 of a planned 380 were randomized within 48 hours of presentation. The major reason for nonrecruitment was receipt of antibiotics (2044 [44.6%] screened patients). Median time from presentation to drug administration was 22 hours (interquartile range, 14-28 hours). Exacerbation characteristics were well balanced across treatment arms and centers. The primary outcome asthma symptom scores were mean (SD), 4.14 (1.38) at exacerbation and 2.09 (1.71) at 10 days for the azithromycin group and 4.18 (1.48) and 2.20 (1.51) for the placebo group, respectively. Using multilevel modeling, there was no significant difference in symptom scores between azithromycin and placebo at day 10 (difference, −0.166; 95% CI, −0.670 to 0.337), nor on any day between exacerbation and day 10. No significant between-group differences were observed in quality-of-life questionnaires or lung function between exacerbation and day 10, or in time to 50% reduction in symptom score. CONCLUSIONS AND RELEVANCEIn this randomized population, azithromycin treatment resulted in no statistically or clinically significant benefit. For each patient randomized, more than 10 were excluded because they had already received antibiotics.TRIAL REGISTRATION clinicaltrials.gov Identifier: NCT01444469

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Azithromycin for Acute Exacerbations of Asthma

et al. 2016

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“…Although parasites can induce specific IgE and activate TLRs through pathogen-associated molecular patterns, chronic allergic inflammation may lead to activation of TLR by damage-associated molecular patterns [30,31]. In addition, certain viral and bacterial infections have been associated with asthma exacerbations [32,33], and the presence of endotoxin (TLR-4 ligand) was demonstrated in house dust, and was related to severity of allergic reactions against house dust mite [21], Our data indicate that activation of basophils may contribute to these processes by enhanced cytokine production when both specific IgE and TLR ligands are present.…”

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Activation of human basophils by combined toll‐like receptor‐ and FcεRI‐triggering can promote Th2 skewing of naive T helper cells

et al. 2013

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Additional supporting information may be found in the online version of this article at the publisher's web-site IntroductionBasophils are circulating granulocytes that can migrate to tissues when inflammation or other triggers are present locally. Activation of basophils through crosslinking of FcεRI via antigen-specific IgE causes the release of granule contents (histamine, proteoglycans), lipid-derived mediators (leukotrienes), and cytokines. Due to their potent activation via IgE-bound antigens and their production of T helper 2 (Th2) type cytokines such as IL-4 and IL-13, Correspondence: Jolien Suurmond e-mail: j.suurmond@lumc.nl basophils are often considered important innate effector cells in IgE-mediated immune responses. Besides activation through IgE, several other pathways have been described to activate basophils, including activation through complement receptors and toll-like receptors (TLR). Although information about TLR protein expression and the response of basophils to TLR ligands is scarce, human basophils express mRNA of several TLRs, and protein of TLR-2 and -4. However, the functional response of basophils to ligation of most TLRs is unknown [1][2][3][4].Basophil responses to TLR ligands may be important, as it is not understood how pathogens and allergens may lead to induction of Th2 responses. As TLR ligation of dendritic cells most often induces type 1 responses through production of IL-12, it is not understood whether and how Th2 cells can be induced via TLR. Since basophils are a known early source of IL-4 and other cytokines associated with Th2 responses, they have been proposed to play a prominent role in the induction of such responses [8]. In mice, it was suggested that basophils play a crucial role in responses against Th2-associated helminth parasites and in protease allergens [9][10][11]. Basophils were proposed to function as APCs in these studies and were also shown to be present in LNs in models of allergy and helminth infection [12][13][14]. However, the function of basophils as APCs during the priming phase of Th2 responses in mice has been challenged by others [13,15,16], and human basophils could not present antigens to CD4 + T cells [17,18]. Therefore, it seems unlikely that human basophils function as APCs. However, by providing an early IL-4 signal that facilitates Th2 skewing after T-cell activation by APCs, basophils could play an important role in skewing of Th2 responses as accessory cells. Indeed, in a mouse model for papain-induced Th2 responses, both DCs and basophils were important for Th2 skewing [19].Since several allergens and helminth parasites can activate TLRs [20][21][22], it would be of high importance to know whether human basophils can be activated via TLR triggering, and if so, which cytokines are released. Until now, little information on these aspects is available for human basophils. Furthermore, as allergic responses and helminth infections may induce IgE responses [23], it would be important to know whether these pathways would interact and prom...

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“…The primary focus has been upon viruses, particularly rhinovirus [2,3], and bystander airway tissue damage during host-antiviral responses is widely believed to play a key role in driving wheezing disease pathogenesis towards chronicity. Considerably less attention has been paid to bacteria, with the exception of Staphylococcus aureus (SA) strains which produce soluble enterotoxins.…”

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Th2-associated immunity to bacteria in teenagers and susceptibility to asthma

Hollams

Hales²,

Bachert³

et al. 2010

Eur Respir J

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Bacterial colonisation of the airways is associated with increased risk of childhood asthma. Immunoglobulin (Ig)E against bacterial antigens has been reported in some asthmatics, suggesting a role for bacterial-specific type-2 immunity in disease pathogenesis. We aimed to investigate relationships between bacterial-specific IgE amongst teenagers and asthma susceptibility.We measured titres of IgE against Haemophilus influenzae, Streptococcus pneumoniae and Staphylococcus aureus in 1,380 teenagers, and related these to asthma symptomatology and immunophenotypes.IgE titres against S. aureus-derived enterotoxins were highest amongst atopics and were associated with asthma risk. Surprisingly, IgE titres against H. influenzae and S. pneumoniae surface antigens were higher, not stratified by atopy and independently associated with decreased asthma risk.The positive association between type-2 immunity to S. aureus and asthma phenotypes probably reflects IgE-mediated effector cell activation via enterotoxin super antigens which are secreted in soluble form. The contrasting benign nature of type-2 immunity to H. influenzae and S. pneumoniae antigens may reflect their lower availability in soluble forms that can crosslink IgE receptors. We theorise that instead they may be processed by antigen presenting cells and presented to type-2 memory cells leading to mucosal secretion of interleukin (IL)-4/IL-13, a mechanism widely recognised in other tissues to attenuate T-helper-1 associated bacterialinduced inflammation.

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Rhinovirus-induced lower respiratory illness is increased in asthma and related to virus load and Th1/2 cytokine and IL-10 production

Cited by 451 publications

References 29 publications

Azithromycin for Acute Exacerbations of Asthma

Azithromycin for Acute Exacerbations of Asthma

Activation of human basophils by combined toll‐like receptor‐ and FcεRI‐triggering can promote Th2 skewing of naive T helper cells

Th2-associated immunity to bacteria in teenagers and susceptibility to asthma

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