Alain Van Muylem

and 6 more

Background: Severe asthma is associated with an accelerated lung function decline which is likely attenuated by the addition of anti-nnterleukin-5 (IL-5) therapy in patients with severe eosinophilic asthma. Objective: To study the long-term impact of add-on therapy with anti-IL-5 on FEV 1 in severe eosinophilic asthma patients. Methods: In this post-hoc analysis, we compared, through a linear mixed model, the evolution of pre-bronchodilation FEV 1 expressed in %pred in a cohort of 50 patients with severe eosinophilic asthma treated with anti-IL-5 (1576 visits) before (median follow-up: 9.2 years) and after (median follow-up: 2.1 years (up to 6.8 years) anti-IL-5 therapy start. Results: FEV 1 decline was observed before anti-IL5 start (-0.6 %pred.year -1, p<0.001). FEV 1 improved significantly after anti-IL-5 start (+1.3 %pred.year -1 p<0.001; difference pre-post: p<0.001). A sustained improvement was observed in 31 patients deemed responders (+3.1 %pred.year -1, p<0.001; difference pre-post: p<0.001) vs a continuous decline in 19 patients considered as non-responders (-0.40 %pred.year -1, p=0.087; difference pre-post: p=0.097). Non-responders exhibited a higher prevalence of nasal polyposis, better asthma control and a trend towards higher exhaled nitric oxide values. Conclusion: This post-hoc analysis shows that add-on therapy with anti-IL-5 not only stems the accelerated decline in lung function but also makes it reversible in many severe eosinophilic asthma patients, leading to an estimated improvement of 11% FEV 1 %pred after 3 years of treatment. Persistent improvement in lung function is therefore feasible in severe asthmatics and could be chosen as a lung function criterion to define remission of asthma under treatment.

Amaryllis Haccuria

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Introduction The IL-33 pathway involved in the development of type-2 airway inflammation is activated in allergic asthma patients. According to the “one airway, one disease” concept, the IL-33 pathway should also be activated in the airways of allergic rhinitis patients. Material and methods We compared the levels of IL-33 and its mRNA precursor, in induced sputum of patients suffering from seasonal allergic rhinitis (n=27) with those measured in patients with seasonal allergic asthma (n=23), and in healthy controls (n=17), in and out of the pollen season. Results IL-33 levels were higher in sputum supernatants of allergic rhinitis (median 9.4 pg.ml-1, range 0 – 51.1 pg.ml-1) and asthma patients (5.2 pg.ml-1, range 0 – 45.4 pg.ml-1) when compared to controls (median 0 pg.ml-1, range 0 – 13 pg.ml-1; p<0.001), and the same was observed with qPCR for IL-33. IL-33 levels were similar in patients suffering from allergic rhinitis (median 4.9 pg.ml-1 vs 7.1 pg.ml-1, p=0.256) or allergic asthma patients (median 3.6 pg.ml-1 vs 3.2 pg.ml-1, p=0.61) in and out of pollen seasons. Conclusion IL-33 is detectable in the lower airways of allergic rhinitis patients, to similar levels than in asthma patients, and appears to be independent of natural variation in allergen exposure. Those findings could reflect a silent epithelial dysfunction in the lower airways of allergic rhinitis patients without asthma, further confirming the «one airway, one disease» theory linking asthma and rhinitis.