Outcome
| Type |
Measure |
Description |
Time frame |
Safety issue |
| Primary |
Inflammatory profile at exacerbation |
concentration levels of IFNg, IL-5, IL-13, IL-33, TSLP in blood and induced sputum (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion |
|
| Secondary |
Inflammatory profile at steady state |
concentration levels of IFNg, IL-5, IL-13, IL-33, TSLP in blood and induced sputum (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
at baseline: consult at least 8 weeks after exacerbation |
|
| Secondary |
Change of inflammatory profile between exacerbation and steady state |
concentration levels of IFNg, IL-5, IL-13, IL-33, TSLP in blood and induced sputum (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Levels of cytokines in blood |
Concentration levels of cytokines (IL-4, IL-17A, IL-22, TNF-alpha, IL-1beta, IL-6, IL-10) in blood (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Levels of cytokines in induced sputum |
Concentration levels of cytokines (IL-4, IL-17A, IL-22, TNF-alpha, IL-1beta, IL-6, IL-10) in induced sputum (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Levels of interferons in blood |
Concentrations levels of interferons (IFN-beta, IL-29) in blood (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Levels of interferons in induced sputum |
Concentration levels of interferons (IFN-beta, IL-29) in induced sputum (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Levels of chemokines in blood |
Concentration levels of chemokines (CXCL8, CXCL10, CCL5, CCL20) in blood (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Levels of chemokines in induced sputum |
Concentration levels of chemokines (CXCL8, CXCL10, CCL5, CCL20) in induced sputum (all concentrations expressed in pg/ml, obtained with multiplex assays) between wheeze patterns: EVW (among which SIW) vs MTW |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Expression patterns of mononuclear cells |
Percentage of mononuclear cells in peripheral blood and sputum (sorted by flow cytometry): lymphocytes, dendritic cells, innate lymphoid cells |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Percentage of patients with tobacco exposure |
Percentage of tobacco exposure (qualitative data) |
At the time of the inclusion |
|
| Secondary |
Percentage of patients with mould/moisture exposure |
Percentage of visible mould/moisture exposure (qualitative data, based on declaration by the parents) |
At the time of the inclusion |
|
| Secondary |
Percentage of patients with pet ownership |
Percentage of pet ownership (qualitative data) |
At the time of the inclusion |
|
| Secondary |
Percentage of patients living in urban area |
Percentage of urban living (qualitative data) |
At the time of the inclusion |
|
| Secondary |
number of asthma exacerbations in the previous year |
number of asthma exacerbations in the previous year (quantitative data) |
At the time of the inclusion |
|
| Secondary |
Percentage of patients with associated atopic diseases |
Percentage of associated atopic disorders: atopic dermatitis, atopic rhinitis, food allergy (qualitative data) |
At the time of the inclusion |
|
| Secondary |
Control of asthma |
Control of asthma based on symptoms (breath, cough, breathlessness, impact on activity and social behavior) and previous exacerbations in the past year, and classified according to GINA criteria: well-controlled, partly controlled, uncontrolled (semi-quantitative) |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Features of the exacerbation: severity |
Severity assessed during the first hour in the emergency department (before treatment), using PRAM severity score: mild asthma (0-3), moderate asthma (4-7), severe asthma (8-12) (quantitative data) |
At the time of the inclusion |
|
| Secondary |
Features of the exacerbation: length |
Length of stay and length of oxygen need (in days) |
At the time of the inclusion |
|
| Secondary |
Atopy |
Atopy: positivity of skin prick tests (= 3 mm diameter) and/or specific IgE (= 0,35 ku/l), mono or polysensitized status (qualitative data) |
At the time of the inclusion and at the age of 7 |
|
| Secondary |
Blood leukocyte count |
Count of neutrophils and eosinophils (number/mm3) |
At the time of the inclusion and at the age of 7 |
|
| Secondary |
ImmunoCAP ISAC (Thermo Fisher Scientific) |
Levels of component specific IgE antibodies will be expressed in ISAC standardized units (ISU). We will categorized the raw data into 4 sIgE semiquantitative discrete groups, according to the manufacturer's guidelines: no (<0.3 ISU), low (0.3-1 ISU), medium (1-15 ISU), and high (>15 ISU) sensitization |
At the time of the inclusion and at the age of 7 |
|
| Secondary |
Microbiological phenotype: viral status |
Virus identification by PCR in nasal swab sample (qualitative data) |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
Microbiological phenotype: bacteriological status |
Positive identification of bacteria (positive if titer >= 10.4/ml) by culture of induced sputum (qualitative data) |
At the time of the inclusion and at baseline (consult at least 8 weeks after exacerbation) |
|
| Secondary |
History at the age of 7 |
History of asthma exacerbations in the previous year, presence of other atopic diseases: atopic dermatitis, atopic rhinitis, food allergy (qualitative data) |
At the age of 7 |
|
| Secondary |
Control of asthma at the age of 7 |
Control of asthma based on symptoms (breath, cough, breathlessness, impact on activity and social behavior) and previous exacerbations in the past year, and classified according to GINA criteria: well-controlled, partly controlled, uncontrolled (semi-quantitative) |
At the age of 7 |
|
| Secondary |
Atopy at the age of 7 |
Atopy: positivity of skin prick tests (= 3 mm diameter) and/or specific IgE (= 0,35 ku/l), mono or polysensitized status (qualitative data) |
At the age of 7 |
|
| Secondary |
Lung function at the age of 7: forced expiratory volume in one second |
Forced expiratory volume in one second (FEV1) after administration of short acting beta agonists, obtain with spirometry test (expressed in Z-score) |
At the age of 7 |
|
| Secondary |
Lung function at the age of 7 : forced vital capacity |
Forced vital capacity (FVC) after administration of short acting beta agonists, obtain with spirometry test (expressed in Z-score) |
At the age of 7 |
|
