Thesis
Fractional exhaled nitric oxide non-suppression in asthma
- Abstract:
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Background: Factional exhaled nitric oxide (FeNO) and blood eosinophils are biomarkers of the higher risk type-2 inflammatory phenotype in asthma.
Objectives: 1) To assess if patients who fail to suppress FeNO after monitored therapy exhibit corticosteroid resistance. 2) To translate non-suppression of type-2 biomarkers to inflammatory mediators in the airway and peripheral blood in severe asthma. 3) To develop a prototype risk scale predicting asthma attacks based on FeNO and blood eosinophils.
Methods: 1) Induced sputum eosinophils and 11 sputum supernatant plus 9 serum inflammatory proteins were analysed in a paired before/after analysis of FeNO suppression tests conducted in Oxford, compared on the basis of a positive/negative test (i.e.: ≥42/% decrease in FeNO following monitored high-intensity corticosteroid therapy). 2) These inflammatory mediators were also correlated to the FeNO and blood eosinophil levels at the point of maximum treatment intensity in a cross-sectional study pooling the Oxford FeNO suppression cohort and the RASP-UK trial cohort. 3) Biomarker-stratified trial-level attack rates were extracted and pooled from the control arms of 8 randomised clinical trials. These were used to derive rate ratios and the predicted asthma attack rate for different patient groups.
Results: 1) Thirty-four FeNO suppression tests were analysed. The 19 patients failing to suppress FeNO were older, more intensely treated, and had little or no trends for improvement in clinical nor sputum/serum measurements compared to those who suppressed. 2) In 74 patients with severe asthma, FeNO correlated with airway type-2 cytokine, chemokine, alarmin and eosinophilia, whilst blood eosinophils correlated with serum interleukin-5. 3) The trial-derived (n=3051) prototype risk scale showed feasibility and potential to predict asthma attacks which can be prevented by anti-inflammatory therapy.
Conclusion: FeNO non-suppression carries significant translational, prognostic and theragnostic utility as a biomarker of type-2 airway inflammation in asthma – especially when used in combination with blood eosinophils.
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(Preview, Dissemination version, pdf, 3.4MB, Terms of use)
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Authors
Contributors
- Institution:
- University of Oxford
- Division:
- MSD
- Department:
- NDM
- Role:
- Supervisor
- Institution:
- University of Oxford
- Division:
- MSD
- Department:
- NDM
- Role:
- Supervisor
- Funder identifier:
- http://dx.doi.org/10.13039/100010269
- Funding agency for:
- Hinks, T
- Grant:
- 211050/Z/18/Z
- Programme:
- Wellcome Trust Senior Fellowship
- Funder identifier:
- http://dx.doi.org/10.13039/100004339
- Funding agency for:
- Hinks, T
- Couillard Castonguay, S
- Pavord, I
- Programme:
- Type-2 innovation grant
- Funder identifier:
- http://dx.doi.org/10.13039/501100000272
- Funding agency for:
- Hinks, T
- Pavord, I
- Programme:
- Oxford respiratory BRC
- Funding agency for:
- Couillard Castonguay, S
- Programme:
- Clinical research fellowship salary award
- DOI:
- Type of award:
- MSc
- Level of award:
- Masters
- Awarding institution:
- University of Oxford
- Language:
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English
- Keywords:
- Subjects:
- Pubs id:
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2043024
- Local pid:
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pubs:2043024
- Deposit date:
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2022-06-23
- ARK identifier:
Terms of use
- Copyright holder:
- Couillard Castonguay, S
- Copyright date:
- 2021
- Licence:
- CC Attribution (CC BY)
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