A Cross-sectional Study to Measure Cough in Severe Asthma

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Belépés Regisztrálás

A hivatkozás a vágólapra kerül

ÁllapotElkészült

Szponzorok

Queen's University, Belfast

Együttműködők

King's College London

KLINIKAI VIZSGÁLAT: NCT03999203

BioSeek: nct03999203

Kulcsszavak

Absztrakt

This study aims to characterise cough in severe asthma through an observational cross-sectional analysis of patients stratified by inflammatory biomarker profile using a number of subjective and objective cough measurement tools.

Leírás

This study will use a combination of subjective and objective cough measures to assess the frequency of cough as well as its related morbidity in severe asthmatics. Comparisons will be made between T2-High, T2-Low and T2-intermediate patients defined using a composite biomarker profile (blood eosinophil count and FeNO) to assess the role of cough in each and these results will be compared to the transcriptomic and proteomic measurements in the RASP-UK where the same biomarker profiling is being used to define clinical sub-groups of severe asthma. This study aims to also improve characterisation of the T2-Low population and identify possible mechanisms for the pathophysiology of this group.

60 patients are expected to be recruited to the study. Patients will be provided with an information sheet and have a telephone follow-up after at least 24 hours to ask if they remain interested in participation and if so, they will then be asked back for a baseline visit.

Three groups of severe asthmatics will be recruited (as described in appropriate section) and undergo the following procedures:

- Demographic details, height, weight, spirometry, FeNO and vital signs

- Patient reported outcomes:

- Asthma Mini-Asthma Quality of Life Questionnaire (mini-AQLQ) - abbreviated version of Juniper AQLQ

- Asthma Control Questionnaire (ACQ-5 (5 questions);

- Leicester Cough Questionnaire, the Cough-specific quality-of-life Questionnaire and Cough Hypersensitivity Questionnaire will be used to assess the impact of cough;

- Visual analogue scales (VAS) for cough (VASc) and urge to cough (VASu) will be used as a measure of cough severity.

- Blood samples - a sample of blood will be taken for whole blood transcriptomic and serum analyses

- Citric acid cough challenge test will be used to measure cough reflex sensitivity in each phenotype.

- Spontaneous sputum sample - if patients produce a sputum sample during spirometry or citric acid challenge, this will be recorded and the sample will be retained for sputum differential cell count and storage of processed soluble components.

- On completing the above procedures, patients will be asked to wear a validated ambulatory cough monitor (Leicester Cough Monitor) for a 24-hour period to assess the frequency of cough and if they agree, will be fully instructed in its use.

Patients will be asked to attend a follow-up visit 2 weeks after baseline. The study procedures will remain the same as visit 1 with the exception of collection of clinical samples.

A mild/moderate population will be recruited and undergo the same procedures as the severe group in a baseline visit. No mild/moderate asthmatics will be asked to attend for a follow-up visit.

Dátumok

Utolsó ellenőrzés:	02/29/2020
Első benyújtás:	04/11/2018
Becsült beiratkozás benyújtva:	06/24/2019
Első közzététel:	06/25/2019
Utolsó frissítés beküldve:	03/02/2020
Utolsó frissítés közzétéve:	03/03/2020
A tanulmány tényleges kezdési dátuma:	10/03/2017
Becsült elsődleges befejezési dátum:	12/29/2019
A tanulmány becsült befejezési dátuma:	12/29/2019

Állapot vagy betegség

Asthma

Cough

Beavatkozás / kezelés

Drug: Citric acid

Device: Leicester Cough monitor

Other: fractional exhaled nitric oxide testing (FeNO)

Other: Patient reported outcome measures

Fázis

Karcsoportok

Kar	Beavatkozás / kezelés
A - T2 High Severe Asthmatics Severe asthmatic patients with consistent eosinophil count ≥ 0.3x10^9/mL and consistently high FeNO levels ≥30 ppb. Interventions include 24 hour ambulatory cough monitoring (Leicester Cough Monitor), citric acid cough challenge, fractional exhaled nitric oxide (FeNO) testing, patient reported outcome measures and blood, urine and sputum sampling
B - T2 Low Severe Asthmatics Severe asthmatic patients with consistent eosinophil count ≤ 0.2x10^9/mL and consistently low FeNO levels <30 ppb. Interventions include 24 hour ambulatory cough monitoring (Leicester Cough Monitor), citric acid cough challenge, fractional exhaled nitric oxide (FeNO) testing, patient reported outcome measures and blood, urine and sputum sampling
C - Mild/Moderate Asthmatics mild/moderate severe asthmatics (defined as step 2/3 using the GINA classification of severity) recruited from general respiratory clinics in the Belfast HSC Trust Interventions include 24 hour ambulatory cough monitoring (Leicester Cough Monitor), citric acid cough challenge, fractional exhaled nitric oxide (FeNO) testing, patient reported outcome measures and blood, urine and sputum sampling
D - T2 Intermediate Severe asthmatic patients with consistent eosinophil count ≥ 0.3x10^9/mL OR consistently high FeNO levels ≥30 ppb. Interventions include 24 hour ambulatory cough monitoring (Leicester Cough Monitor), citric acid cough challenge, fractional exhaled nitric oxide (FeNO) testing, patient reported outcome measures and blood, urine and sputum sampling

Jogosultsági kritériumok

Tanulásra alkalmas korok	18 Years Nak nek 18 Years
Tanulásra alkalmas nemek	All
Mintavételi módszer	Non-Probability Sample
Egészséges önkénteseket fogad	Igen
Kritériumok	Inclusion Criteria (Severe Asthmatics): 1. Ability and willingness to comply with the study procedures 2. Age ≥18 to ≤75 years at the time of informed consent 3. Severe asthma (as defined by GINA step 4/5 classification of asthma severity) after a detailed systematic assessment 4. History of asthma treatment with high doses of Inhaled Corticosteroids (≥1000 µg beclomethasone dipropionate daily, or equivalent) and an additional controller 5. Three patient groups with severe asthma will be investigated in the study and will be defined as follows: T2-High Severe Asthmatics (Group A) - Persistent blood eosinophil count ≥0.3x10^9/mL and - Persistent high FeNO levels ≥30 ppb and - Adherence to inhaled and oral corticosteroid therapy T2-Low Severe Asthmatics (Group B) - Persistent blood eosinophil count ≤0.2x10^9/Ml and - Persistent low FeNO levels (<30ppb) T2 - Intermediate Severe Asthmatics (Group D) - Persistent blood eosinophil count ≥ 0.3x10^9/mL OR - Persistent FeNO levels ≥ 30 ppb As stated above, these measurements are made at each clinic visit as part of routine care and will be available on all subjects prior to Inclusion 6. A chest x-ray or CT scan obtained within 12 months before the time of informed consent and showing no new pathology requiring investigation as a potential cause for their cough Mild/moderate severe asthmatics (who have received a diagnosis of asthma from a physician and are defined as step 2/3 using the BTS/SIGN classification of severity and ACQ<1.5) aged 18-75 years inclusive will be recruited from general respiratory clinics in the Belfast HSC Trust. Patients must have the ability and willingness to comply with study procedures. Exclusion Criteria: 1. Baseline FEV1 ≤50% of predicted or ≤ 1.0L 2. Asthma exacerbation within 28 days before the time of informed consent or during screening 3. Major episode of infection requiring any of the following: - Admission to hospital for ≥24 hours within the 28 days before the time of informed consent - Treatment with intravenous antibiotics within the 28 days before the time of informed consent or during Screening - Treatment with oral antibiotics within the 14 days before the time of informed consent or during Screening 4. For adults: Active tuberculosis (TB) requiring treatment within the 12 months before the time of informed consent (patients are also required to have no recurrence of symptoms in the 12 months following completion of TB treatment), or 5. Known history of severe clinically significant immunodeficiency, including, but not limited to, human immunodeficiency virus infection and/or currently receiving or have historically received intravenous Ig for treatment for immunodeficiency Note: Immunodeficiency encompasses a wide spectrum of human conditions and/or diseases. A relative IgG deficiency that is thought, but not proven, to be a feature of severe asthma would not be exclusionary for the study. 6. Diagnosis or history of malignancy, or current investigation for possible malignancy 7. Other clinically significant medical disease that is uncontrolled despite treatment or that is likely, in the opinion of the investigator, to require a change in therapy or affect the ability to participate in the study 8. History of alcohol, drug, or chemical abuse that would impair or risk the patient's full participation in the study, in the opinion of the investigator 9. Current smoker or former smoker with a smoking history of >15 pack-years A current smoker is defined as someone who has smoked one or more cigarettes per day (or marijuana or pipe or cigar) for ≥30 days within the 24 months before the time of informed consent and for whom cotinine testing is positive. A former smoker is defined as someone who has smoked one or more cigarettes per day (or marijuana or pipe or cigar) for ≥30 days in his or her lifetime (as long as the 30-day total did not include the 24 months before the time of informed consent) and for whom cotinine testing is negative. A pack-year is defined as the average number of packs per day times the number of years of smoking. 10. Initiation of or change in allergen immunotherapy within three months before the time of informed consent 11. Treatment with an investigational agent within 30 days of informed consent or 5 half-lives of the investigational agent, whichever is longer 12. Female patients who are pregnant or lactating

Eredmény

Elsődleges eredménymérők

1. Cough frequency measurement [Baseline]

Objectively measure cough frequency in different phenotypes of severe asthma and a mild/moderate control group using a validated ambulatory cough monitor (Leicester Cough Monitor)

2. Cough Reflex sensitivity [Baseline]

To objectively measure cough reflex sensitivity in different phenotypes of severe asthma and a mild.moderate control group using citric acid cough challenge testing

Másodlagos eredménymérők

1. Reproducibility [Baseline and 2 weeks]

Reproducibility of objective and subjective measures of cough in a severe asthma population will be explored.

2. Asthma Control Questionnaire [Baseline]

Assessment of asthma control using subjective questionnaire (asthma control questionnaire) in different phenotypes of severe asthma. Patient responses graded on likert scale with an average score being calculated. A higher score indicates a worse level of asthma control. Score range 0-6

3. Asthma Quality of Life Questionnaire [Baseline]

Assesment of quality of life in asthma as perceived by the patient using this questionnaire in different phenotypes of severe asthma. Patient responses graded on likert scale with an average score being calculated. A higher score indicates a worse level of asthma related quality of life. Score range 1-7

4. Leceister Cough Questionnaire [Baseline]

Assessment of quality of life in relation to cough in different phenotypes of severe asthma. Patient responses graded on likert scale with an average score being calculated from different symptoms domains wihtin the questionnaire. A lower score indicates a worse level of cough related quality of life. Score range 3-21

5. Cough Quality of Life Questionnaire [Baseline]

Assessment of quality of life in relation to cough in different phenotypes of severe asthma. Patient responses graded on likert scale with a total score being calculated. A higher score indicates a worse level of cough related quality of life. Score range 28-112

6. Visual Analogue Scale for Cough Severity [Baseline]

Visual analogue scale where patients are asked to mark on a scale of 0-100 how severe they perceive their cough. Score range 0 (no cough) to 100 (worst cough possible)

7. Visual analogue scale for urge to cough [Baseline]

Visual analogue scale where patients are asked to mark on a scale of 0-100 how severe they perceive their urge tocough. Score range 0 (no urge to cough) to 100 (worst urge to cough possible)

8. Cough Hypersensitvity Questionnaire [Baseline]

Questionnaire which evaluates the presence of cough triggers, urge to cough and laryngeal symptoms suggestive of neuropathic paraesthesia. Score range 0-150

9. Relationship between cough frequency and blood eosinophils [Baseline]

To determine the relationship between cough frequency count and blood eosinophils count (x10^9 / L)

10. Relationship between cough frequency and asthma control questionnaire [Baseline]

o determine the relationship between cough frequency count and asthma control questionnaire score (0-5)

11. Relationship between cough frequency and Fractional Exhaled Nitric Oxide (FeNO) [Baseline]

o determine the relationship between cough frequency count and FeNO (measured in parts per billion (ppb))

12. Relationship between leicester cough questionnaire and blood eosinophils [Baseline]

To determine relationship between cough quality of life and blood eosinophil count (x10^9/L)

13. Relationship between leicester cough questionnaire and asthma control questionnaire [Baseline]

To determine relationship between cough quality of life and asthma control questionnaire score (0-5)

A Cross-sectional Study to Measure Cough in Severe Asthma

Kulcsszavak

gyulladás

hypersensitivity

asztma

köhögés

citric acid

közönséges boróka