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Defining the Severe Paediatric Asthma Endotype (SevAsthma)

Primary Purpose

Severe Asthma

Status
Recruiting
Phase
Not Applicable
Locations
France
Study Type
Interventional
Intervention
Blood collection
Saliva sample
Nasal
Sponsored by
Assistance Publique - Hôpitaux de Paris
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional other trial for Severe Asthma focused on measuring Asthma, Severe, Immunologic, Metabolomic, Microbiologic profil

Eligibility Criteria

undefined - 12 Years (Child)All SexesDoes not accept healthy volunteers

Patient Inclusion Criteria:

  • Minors aged 0 to 6 years or 6 to 12 years, hospitalized for assessment of Severe Asthma
  • Minors need with his follow-up an bronchial endoscopy with realization of LBA and biopsies of bronchial mucosa
  • Social insurance affiliation, except AME
  • Parents or legal guardians signed the Informed consent form

Control Inclusion Criteria:

  • Minors aged 0 to 6 years or 6 to 12 years, hospitalized for assessment of severe respiratory syndrome except severe asthma
  • Minors need with his follow-up an bronchial endoscopy with realization of LBA and biopsies of bronchial mucosa
  • Social insurance affiliation, except AME
  • Parents or legal guardians signed the Informed consent form

Patient Exclusion Criteria

  • Prematurity (<37 weeks gestation)
  • Broncho-pulmonary dysplasia, immune deficits, non-Severe Asthma bronchopathies, cystic fibrosis, heart disease, ongoing biotherapy

Sites / Locations

  • Name: Hôpital Necker-Enfants MaladesRecruiting

Arms of the Study

Arm 1

Arm 2

Arm Type

Other

Other

Arm Label

Cases with SA, classified by age group

Controls among children w/ SA: frequent&infrequent exacerbators

Arm Description

Patient hospitalized for assessment of severe asthma

Frequent exacerbators have 2 or more asthma severe exacerbations in the past years

Outcomes

Primary Outcome Measures

Description of the environment and smoke exposure
Environment Living in a urban or non-urban area : n (%) Visible mold/dampness at home: n (%) Pet ownership: : n (%) Smoke exposure : n (%) Presence of pets at home : n (%)
Description of family atopy status
Atopy in 1 or 2 parents or siblings: n (%) Parental asthma : n (%) Parental atopic dermatitis: n (%) Parental immediate food allergy: n (%) Parental allergic rhinitis: n (%) Asthma in siblings: n (%) Atopic dermatitis in siblings: n (%) Immediate food allergy in siblings: n (%) Allergic rhinitis in siblings: n (%)
Description of Demographics
Sex male or female: n (%) Age at inclusion: y Weight (kg) Height (m) Body mass index : calculated from weight and height Atopy : n (%) Total IgE : n (%) 1 positive allergy tests (SPT or sp IgE) to airborne allergens : n (%) 1 positive SPT or sp IgE to food allergen: n (%) History of food allergy: n (%) History of allergic rhinitis: n (%) History of atopic dermatitis: n (%) Symptomatic gastro-oesophageal reflux: n (%)
Description of Asthma history in the past year
No of severe exacerbations : n ≥ 2 or 3 severe exacerbations: n (%) No. of cumulated days of oral steroids: n No. of emergency visits for acute asthma : n Asthma control ACT score : n
Description of Lung function
Lung function FEV1 pre-BD (% predicted) FEV1 post-BD (% predicted) FEV1 pre-BD (Zscore) FEV1 post-BD (Zscore) FEV1/FVC pre-BD (%) FEV1/FVC post-BD (%) FEV1/FVC pre-BD (Zscore) FEV1/FVC post-BD (Zscore) Post BD FEV1 reversibility (%) No of patients with reversibility : n (%) FeNO (ppb) Asthma therapy ICS : (%) ICS doses : µg/day. eq Budesonide ICS + LABA : n (%) Leukotriene modifier : n (%) Maintenance oral corticosteroids: n (%) Immunotherapy: n (%) Omalizumab or biologics: n (%)
Description of Asthma therapy
ICS : (%) ICS doses : µg/day. eq Budesonide ICS + LABA : n (%) Leukotriene modifier : n (%) Maintenance oral corticosteroids: n (%) Immunotherapy: n (%) Omalizumab or biologics: n (%)
Description of Airway remodeling
reticular basement membrane thickness expressed in µm; airway smooth muscle area ; epithelial integrity; vessel number; mucus gland area
Description of inflammatory and histological features in bronchoalveolar lavages (BAL)
Number of eosinophils, neutrophils, macrophages, basophils, lymphocytes expressed as percentage of total cells in BAL
Description of inflammatory and histological features in bronchial mucosa
Number of eosinophils, neutrophils, macrophages, basophils, lymphocytes expressed per square millimeters of submucosal area
Bronchial mucosa analysis
The number of IgE stained with anti-IgE Ab in the submucosa and the epithelium will be assessed and expressed per square millimeters of submucosal area The expression of cytokines in the mucosa will be assessed by multiplex and expressed in pg/ml or ng/ml. Quantify by quantitative PCR mRNA encoding cytokines, chemokines and others immune activation markers as relative mRNA levels.
BAL analysis
The number of mast cells, lymphocytes, innate lymphoid cells, mucosalassosiated invariant T (MAIT) cells, gammadelta T cells expressed as percentage of total cells in BAL, concentrations of Immunoglobulins G, E, M will be assessed and express in Ku/L The expression of cytokines will be assessed by multiplex and expressed in pg/ml or ng/ml.
Blood analysis
Number of eosinophils, neutrophils, macrophages, basophils, lymphocytes, innate lymphoid cells expressed as percentage of total cells in blood; number of mucosal associated invariant T (MAIT) cells will be assessed and expressed as percentage of total cells and T cells in blood The number of invariant natural killer T cells will be assessed and expressed as percentage of total cells and T cells in blood The number of gammadelta T cells will be assessed and expressed as percentage of total cells and T cells in blood The concentrations of Immunoglobulins G, E, M will be assessed and express in Ku/L The expression of cytokines will be assessed by multiplex and expressed in pg/ml or ng/ml.
Metabolomic signature
The global concentration of metabolites is first expressed as the signal intensity compared to internal controls. When metabolites are identified, they are quantified and their concentration expressed as pg/ml.
Microbiota analysis
Quantify by quantitative PCR mRNA and DNA encoding as relative mRNA and DNA levels

Secondary Outcome Measures

Cluster analysis
Identify the main phenotypes of severe asthma by the cluster analysis.
Number of severe exacerbations in the 12 months following the inclusion
Patients will be then categorized in frequent exacerbators and non-frequent exacerbators (n) according to their number of severe exacerbations in the 12 months following inclusion
Asthma Control Test (ACT) score 12 months after inclusion
from 0 to 27 (for children 4-11 years); from 5-25 for children 12 years and older - higher score is better control
Asthma control 12 months after inclusion
according to international guidelines : not controlled, partially controlled, controlled
Description of lung function 12 months after the inclusion
FEV1 pre-BD (% predicted); FEV1 post-BD (% predicted); FEV1 pre-BD (Zscore); FEV1 post-BD (Zscore); FEV1/FVC pre-BD (%); FEV1/FVC post-BD (%); FEV1/FVC pre-BD (Zscore); FEV1/FVC post-BD (Zscore); Post BD FEV1 reversibility (%); No of patients with reversibility : n (%); FeNO (ppb)
Number of severe exacerbations during the 1 year follow up
Number of emergency department visits for acute asthma during the 1 year follow up
Number of cumulated days of oral steroids for asthma exacerbations during the 1 year follow up
Number of hospital admissions for acute asthma during the 1 year follow up

Full Information

First Posted
September 14, 2020
Last Updated
October 28, 2022
Sponsor
Assistance Publique - Hôpitaux de Paris
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1. Study Identification

Unique Protocol Identification Number
NCT04680117
Brief Title
Defining the Severe Paediatric Asthma Endotype
Acronym
SevAsthma
Official Title
Defining the Severe Paediatric Asthma Endotype: an Integrated Approach Combining Phenotypic Analyses Related to Immune, Metabolomics and Microbial Features
Study Type
Interventional

2. Study Status

Record Verification Date
October 2022
Overall Recruitment Status
Recruiting
Study Start Date
June 15, 2021 (Actual)
Primary Completion Date
January 2025 (Anticipated)
Study Completion Date
January 2025 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Assistance Publique - Hôpitaux de Paris

4. Oversight

Studies a U.S. FDA-regulated Drug Product
No
Studies a U.S. FDA-regulated Device Product
No
Data Monitoring Committee
No

5. Study Description

Brief Summary
The primary objective of this project is to extensively characterize the endotypes of pre-schoolers (0 to 6 years) and school-age children (6 to 12 years) with SA using an integrated approach, combining a description of their phenotype (asthma symptoms, atopy, and lung function) associated with histological (airway inflammation and remodelling), immune (innate and adaptive immunity), metabolomics, and microbiota analyses. This goal shall be achieved by an unsupervised in-depth analysis of patients requiring bronchial endoscopy, with bronchial alveolar lavage (BAL) and bronchial biopsy, as part of their clinical assessment.
Detailed Description
Asthma is a chronic disease affecting approximately 235 million people worldwide, and the number is rising. Asthma is not just a public health problem for developed countries; its incidence is also elevated in developing countries. Asthma concerns all age groups, but often starts in childhood. SA in children is infrequent, affecting 2-5% of the asthmatic paediatric population. Children with SA experience frequent SA attacks and have a reduced quality of life . They account for approximately half of the asthma healthcare costs. Asthma has long been thought to be a single disease but is now considered to encompass various conditions characterized by the same symptoms (wheeze, cough, shortness of breath, chest tightness), variable degrees of airflow limitation, and different pattern of inflammation. Recent studies highlighted the heterogeneity of asthma, and the potential influence of various pathogenic mechanisms, including airway inflammation, remodelling, and immune and metabolic pathways in a specific microbial environment. However, there is very little data concerning the pathological process, especially in children. Most of the data describing different asthma endotypes in children are derived from large observational prospective cohorts. Although very informative, these studies were designed to analyse a small number of easily measured parameters, mainly lung function and atopy. The complexity of asthma pathogenesis was therefore underestimated and the individuals' specificities only partially considered. In clinical practice, children with SA require an endoscopy, with broncho-alveolar lavage fluids (BALF) collection and bronchial biopsies to exclude a differential diagnosis and assess airway inflammation and remodelling. This approach also underestimates other components of the endotypes and results in "one size fits all" management based on high doses of inhaled steroids and the use of expensive biotherapy, such as anti-IgE therapy. Thus, although hospital admission and mortality ratesfor asthma decreased until the early 2000's, they have remained stable over the past 10 years. It is therefore imperative to develop new approaches that incorporate relevant parameters analysed in the airways. This project proposes an in-depth analysis, not only of clinical and functional parameters, but also of immune cells, metabolomic compounds, and microbiota present in the airways of asthmatic children. The primary objective of the project is to extensively characterize the endotypes of pre-schoolers (0 to 6 years) and school-age children (6 to 12 years) with SA using an integrated approach, combining a description of their phenotype (asthma symptoms, atopy, and lung function) associated with histological (airway inflammation and remodelling), immune (innate and adaptive immunity), metabolomics, and microbiota analyses. This goal shall be achieved by an unsupervised in-depth analysis of patients requiring bronchial endoscopy, with bronchial alveolar lavage (BAL) and bronchial biopsy, as part of their clinical assessment. The main hypothesis is that the complementarity of those approaches will allow investigators to delineate the immune and metabolic pathways and microbiota involved in children with SA. The secondary objectives are to: (1) cluster all data obtained to define new patient groups and develop biomarkers that summarise the different clusters; (2) determine the immune, metabolomic, and microbiota profile of these children to aid future fundamental research that will focus on dissecting new mechanisms involved in paediatric asthma; (3) determine whether pre-schoolers and school-age children with SA share common endotypic features; and (4) establish the basis for the prospective follow-up of patients to identify endotypes that predict asthma persistence throughout childhood, severity, and response to treatment.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Severe Asthma
Keywords
Asthma, Severe, Immunologic, Metabolomic, Microbiologic profil

7. Study Design

Primary Purpose
Other
Study Phase
Not Applicable
Interventional Study Model
Parallel Assignment
Masking
None (Open Label)
Allocation
Non-Randomized
Enrollment
150 (Anticipated)

8. Arms, Groups, and Interventions

Arm Title
Cases with SA, classified by age group
Arm Type
Other
Arm Description
Patient hospitalized for assessment of severe asthma
Arm Title
Controls among children w/ SA: frequent&infrequent exacerbators
Arm Type
Other
Arm Description
Frequent exacerbators have 2 or more asthma severe exacerbations in the past years
Intervention Type
Other
Intervention Name(s)
Blood collection
Intervention Description
Blood collection with samples of 15ml max by subject (case or control) at J0, M6 and M12: subject less than 5 kg : 1.8 to 4.5 ml max subject 5 kg to 10 kg : 4.5 to 9 ml max subject 10 kg to 15 kg : 9 to 13.5 ml subject 15 kg to 20 kg : 13.5 to 15 ml max
Intervention Type
Other
Intervention Name(s)
Saliva sample
Intervention Description
Saliva sample by subject at J0
Intervention Type
Other
Intervention Name(s)
Nasal
Intervention Description
Nasal brushing by subject at J0
Primary Outcome Measure Information:
Title
Description of the environment and smoke exposure
Description
Environment Living in a urban or non-urban area : n (%) Visible mold/dampness at home: n (%) Pet ownership: : n (%) Smoke exposure : n (%) Presence of pets at home : n (%)
Time Frame
1 day
Title
Description of family atopy status
Description
Atopy in 1 or 2 parents or siblings: n (%) Parental asthma : n (%) Parental atopic dermatitis: n (%) Parental immediate food allergy: n (%) Parental allergic rhinitis: n (%) Asthma in siblings: n (%) Atopic dermatitis in siblings: n (%) Immediate food allergy in siblings: n (%) Allergic rhinitis in siblings: n (%)
Time Frame
1 day
Title
Description of Demographics
Description
Sex male or female: n (%) Age at inclusion: y Weight (kg) Height (m) Body mass index : calculated from weight and height Atopy : n (%) Total IgE : n (%) 1 positive allergy tests (SPT or sp IgE) to airborne allergens : n (%) 1 positive SPT or sp IgE to food allergen: n (%) History of food allergy: n (%) History of allergic rhinitis: n (%) History of atopic dermatitis: n (%) Symptomatic gastro-oesophageal reflux: n (%)
Time Frame
1 day
Title
Description of Asthma history in the past year
Description
No of severe exacerbations : n ≥ 2 or 3 severe exacerbations: n (%) No. of cumulated days of oral steroids: n No. of emergency visits for acute asthma : n Asthma control ACT score : n
Time Frame
1 day
Title
Description of Lung function
Description
Lung function FEV1 pre-BD (% predicted) FEV1 post-BD (% predicted) FEV1 pre-BD (Zscore) FEV1 post-BD (Zscore) FEV1/FVC pre-BD (%) FEV1/FVC post-BD (%) FEV1/FVC pre-BD (Zscore) FEV1/FVC post-BD (Zscore) Post BD FEV1 reversibility (%) No of patients with reversibility : n (%) FeNO (ppb) Asthma therapy ICS : (%) ICS doses : µg/day. eq Budesonide ICS + LABA : n (%) Leukotriene modifier : n (%) Maintenance oral corticosteroids: n (%) Immunotherapy: n (%) Omalizumab or biologics: n (%)
Time Frame
1 day
Title
Description of Asthma therapy
Description
ICS : (%) ICS doses : µg/day. eq Budesonide ICS + LABA : n (%) Leukotriene modifier : n (%) Maintenance oral corticosteroids: n (%) Immunotherapy: n (%) Omalizumab or biologics: n (%)
Time Frame
1 day
Title
Description of Airway remodeling
Description
reticular basement membrane thickness expressed in µm; airway smooth muscle area ; epithelial integrity; vessel number; mucus gland area
Time Frame
1 day
Title
Description of inflammatory and histological features in bronchoalveolar lavages (BAL)
Description
Number of eosinophils, neutrophils, macrophages, basophils, lymphocytes expressed as percentage of total cells in BAL
Time Frame
1 day
Title
Description of inflammatory and histological features in bronchial mucosa
Description
Number of eosinophils, neutrophils, macrophages, basophils, lymphocytes expressed per square millimeters of submucosal area
Time Frame
1 day
Title
Bronchial mucosa analysis
Description
The number of IgE stained with anti-IgE Ab in the submucosa and the epithelium will be assessed and expressed per square millimeters of submucosal area The expression of cytokines in the mucosa will be assessed by multiplex and expressed in pg/ml or ng/ml. Quantify by quantitative PCR mRNA encoding cytokines, chemokines and others immune activation markers as relative mRNA levels.
Time Frame
1 day
Title
BAL analysis
Description
The number of mast cells, lymphocytes, innate lymphoid cells, mucosalassosiated invariant T (MAIT) cells, gammadelta T cells expressed as percentage of total cells in BAL, concentrations of Immunoglobulins G, E, M will be assessed and express in Ku/L The expression of cytokines will be assessed by multiplex and expressed in pg/ml or ng/ml.
Time Frame
1 day
Title
Blood analysis
Description
Number of eosinophils, neutrophils, macrophages, basophils, lymphocytes, innate lymphoid cells expressed as percentage of total cells in blood; number of mucosal associated invariant T (MAIT) cells will be assessed and expressed as percentage of total cells and T cells in blood The number of invariant natural killer T cells will be assessed and expressed as percentage of total cells and T cells in blood The number of gammadelta T cells will be assessed and expressed as percentage of total cells and T cells in blood The concentrations of Immunoglobulins G, E, M will be assessed and express in Ku/L The expression of cytokines will be assessed by multiplex and expressed in pg/ml or ng/ml.
Time Frame
1 day
Title
Metabolomic signature
Description
The global concentration of metabolites is first expressed as the signal intensity compared to internal controls. When metabolites are identified, they are quantified and their concentration expressed as pg/ml.
Time Frame
1 day
Title
Microbiota analysis
Description
Quantify by quantitative PCR mRNA and DNA encoding as relative mRNA and DNA levels
Time Frame
1 day
Secondary Outcome Measure Information:
Title
Cluster analysis
Description
Identify the main phenotypes of severe asthma by the cluster analysis.
Time Frame
1 year
Title
Number of severe exacerbations in the 12 months following the inclusion
Description
Patients will be then categorized in frequent exacerbators and non-frequent exacerbators (n) according to their number of severe exacerbations in the 12 months following inclusion
Time Frame
1 year
Title
Asthma Control Test (ACT) score 12 months after inclusion
Description
from 0 to 27 (for children 4-11 years); from 5-25 for children 12 years and older - higher score is better control
Time Frame
1 year
Title
Asthma control 12 months after inclusion
Description
according to international guidelines : not controlled, partially controlled, controlled
Time Frame
1 year
Title
Description of lung function 12 months after the inclusion
Description
FEV1 pre-BD (% predicted); FEV1 post-BD (% predicted); FEV1 pre-BD (Zscore); FEV1 post-BD (Zscore); FEV1/FVC pre-BD (%); FEV1/FVC post-BD (%); FEV1/FVC pre-BD (Zscore); FEV1/FVC post-BD (Zscore); Post BD FEV1 reversibility (%); No of patients with reversibility : n (%); FeNO (ppb)
Time Frame
1 year
Title
Number of severe exacerbations during the 1 year follow up
Time Frame
1 year
Title
Number of emergency department visits for acute asthma during the 1 year follow up
Time Frame
1 year
Title
Number of cumulated days of oral steroids for asthma exacerbations during the 1 year follow up
Time Frame
1 year
Title
Number of hospital admissions for acute asthma during the 1 year follow up
Time Frame
1 year

10. Eligibility

Sex
All
Maximum Age & Unit of Time
12 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Patient Inclusion Criteria: Minors aged 0 to 6 years or 6 to 12 years, hospitalized for assessment of Severe Asthma Minors need with his follow-up an bronchial endoscopy with realization of LBA and biopsies of bronchial mucosa Social insurance affiliation, except AME Parents or legal guardians signed the Informed consent form Control Inclusion Criteria: Minors aged 0 to 6 years or 6 to 12 years, hospitalized for assessment of severe respiratory syndrome except severe asthma Minors need with his follow-up an bronchial endoscopy with realization of LBA and biopsies of bronchial mucosa Social insurance affiliation, except AME Parents or legal guardians signed the Informed consent form Patient Exclusion Criteria Prematurity (<37 weeks gestation) Broncho-pulmonary dysplasia, immune deficits, non-Severe Asthma bronchopathies, cystic fibrosis, heart disease, ongoing biotherapy
Central Contact Person:
First Name & Middle Initial & Last Name or Official Title & Degree
Guillaume Lezmi, Doctor (PHU)
Phone
+33 1 44 49 48 38
Email
guillaume.lezmi@aphp.fr
First Name & Middle Initial & Last Name or Official Title & Degree
Sandra Colas
Phone
+33 1 71 19 64 32
Email
sandra.colas@aphp.fr
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Guillaume Lezmi, Doctor (PHU)
Organizational Affiliation
Assistance Publique - Hôpitaux de Paris
Official's Role
Principal Investigator
Facility Information:
Facility Name
Name: Hôpital Necker-Enfants Malades
City
Paris
ZIP/Postal Code
75015
Country
France
Individual Site Status
Recruiting
Facility Contact:
First Name & Middle Initial & Last Name & Degree
Guillaume Lezmi, Doctor (PHU)
Phone
+33 1 44 49 48 38
Email
guillaume.lezmi@aphp.fr

12. IPD Sharing Statement

Plan to Share IPD
No

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Defining the Severe Paediatric Asthma Endotype

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