A 52-week Clinical Trial to Study the Effect of Dexpramipexole in Adolescents and Adults With Severe Eosinophilic Asthma (EXHALE-3)

2023-503693-20-00 Protocol AR-DEX-22-02 Therapeutic confirmatory (Phase III) Not authorised

Status Not authorised · 1 EU/EEA countries · 6 sites · Protocol AR-DEX-22-02

Overview

Sponsor-declared trial summary

Phase Therapeutic confirmatory (Phase III)
Status Not authorised
Participants planned 854
Countries 1
Sites 6

Severe eosinophilic asthma

The primary objective of the study is to demonstrate the efficacy of dexpramipexole in reducing severe asthma exacerbations.

Key facts

Sponsor
Areteia Therapeutics Inc.
Participant type
Pediatric, Patients
Age range
0-17 years, 18-64 years, 65+ years
Gender
Male and Female
Therapeutic area
Diseases [C] - Respiratory Tract Diseases [C08]
Decision date (initial)
2023-09-12
Transition trial
No
Low-intervention
No
Rare-disease indication
No
Vulnerable population
Yes
Funding sources
Areteia Therapeutics, Inc.

External identifiers

EU CT number
2023-503693-20-00
WHO UTN
U1111-1288-9273
ClinicalTrials.gov
NCT05813288

Trial design

CTIS Part I — objectives, methods, condition coding

Main objective

Scope: Safety, Efficacy

The primary objective of the study is to demonstrate the efficacy of dexpramipexole in reducing severe asthma exacerbations.

Secondary objectives 3

  1. To demonstrate the efficacy of dexpramipexole on pulmonary function.
  2. To demonstrate the efficacy of dexpramipexole on asthma control and quality of life
  3. To evaluate the effect of dexpramipexole on blood eosinophils

Conditions and MedDRA coding

Severe eosinophilic asthma

VersionLevelCodeTermSystem organ class
21.1 LLT 10068462 Eosinophilic asthma 10038738

Study design 3 periods

#TitleAllocationBlindingRoles blindedArms
1 Screening Phase: Screening Visit 1 to Baseline.
Screening Visit 1: Participants will undergo screening to assess whether they satisfy the eligibility criteria. Screening Visit 2: Participants will take part in the Run-in Phase (Screening Visit 2 to Baseline; up to 21 days duration, with a minimum of 14 days) as part of the Screening period, to confirm if their current asthma medication regimen is stable.
 Not Applicable None
2 Treatment Phase: Baseline through completion of Week 52 Visit.
Participant eligibility will be assessed during the Screening visits and confirmed at the Baseline Visit. After the collection of all Baseline assessments, participants will begin investigational treatment (dexpramipexole 75 mg, 150 mg, or placebo), BID for 52 weeks. The last dose of investigational product will be taken the evening before the Week 52 Visit. The Week 52 Visit is the Primary Outcome Visit for the study.
 Randomised Controlled Double [{"id":22975,"code":5,"name":"Carer"},{"id":22974,"code":3,"name":"Monitor"},{"id":22977,"code":4,"name":"Analyst"},{"id":22978,"code":2,"name":"Investigator"},{"id":22976,"code":1,"name":"Subject"}]
3 Follow-up Phase: Conclusion of Week 52 assessments through Week 56.
During this phase, participants will have one final phone visit to collect final safety assessments following cessation of investigational product. This visit will occur for any participant not choosing to enroll in the long-term extension study or who discontinues the study early.
 Randomised Controlled Double [{"id":22982,"code":1,"name":"Subject"},{"id":22981,"code":2,"name":"Investigator"},{"id":22984,"code":4,"name":"Analyst"},{"id":22980,"code":3,"name":"Monitor"},{"id":22983,"code":5,"name":"Carer"}]

Regulatory references

Scientific advice from competent authorities
European Medicines Agency
EMA paediatric investigation plan (PIP)
EMEA-003328-PIP01-22

Eligibility criteria

Principal inclusion / exclusion criteria as submitted by sponsor

Inclusion criteria 11

  1. Signed informed consent form and assent form, as appropriate.
  2. Male or female ≥12 years of age at Screening Visit 1.
  3. Documented physician diagnosis of asthma for ≥12 months prior to Screening Visit 1.
  4. Eosinophil count of ≥0.30x109/L at Screening Visit 1. If the initial value is between 0.250x109/L to 0.299x109/L, then this may be repeated once at an unscheduled visit (prior to Screening Visit 2).
  5. Treatment of asthma, participants must satisfy all the below (items a to c): a. Participants who have received asthma controller medication with medium or high dose inhaled corticosteroids (ICS; ≥500 μg/day fluticasone propionate dry powder formulation daily or clinically comparable, per GINA 2021) on a regular basis for at least 12 months prior to Screening Visit 1. Equivalent medium and high dose ICS doses are detailed in Appendix C b. Documented treatment with a stable dose of either medium or high dose ICS for at least 3 months prior to Screening Visit 1. The ICS may be contained within an ICS/long-acting β2 agonist (LABA) combination product. As noted in Section 5.2.2, daily oral corticosteroids are an allowed concomitant medication; participants on daily oral corticosteroids must be on a stable dose for 3 months before Screening Visit 1. c. Use of one or more additional daily maintenance asthma controller medications according to standard practice of care is required; eg, LABA, leukotriene antagonist, theophylline, long-acting muscarinic antagonists, cromolyn/nedocromil. Use of a stable dose of any additional asthma controller medications must be documented for at least 3 months prior to Screening Visit 1.
  6. Pre-BD FEV1 ≥40% and <80% (<90% for participants 12 to 17 years of age) of predicted at Screening Visit 2.
  7. Variable airflow obstruction documented with at least one of the following criteria: a. Bronchodilator reversibility at Screening Visit 2, as evidenced by ≥12% and ≥200 mL improvement in FEV1, 15 to 30 minutes following inhalation of 400 μg (four puffs) of albuterol/salbutamol (≥12% and ≥160 mL for ages 12 to 17). Participants who do not meet the bronchodilator reversibility inclusion criterion but have ≥10% and ≥160 mL reversibility, may repeat the reversibility spirometry assessment once during the Screening period, at an unscheduled visit at least 7 days prior to baseline. b. Bronchodilator reversibility, using the criteria above, documented in the past 24 months prior to Screening Visit 1. c. Peak flow variation of ≥20% over a 2-week period, documented in the past 24 months prior to Screening Visit 1. d. Airflow variability in clinic FEV1 ≥20% between two consecutive clinic visits, documented in the past 24 months prior to Screening Visit 1. e. Airway hyperresponsiveness (provocative concentration causing a 20% fall in FEV1 of methacholine <8 mg/mL) documented in the past 24 months prior to Screening Visit 1.
  8. ACQ-6 ≥1.5 at Screening Visit 2.
  9. Documented history of at least two asthma exacerbations requiring treatment with systemic corticosteroids (intramuscular, intravenous, or oral) within the past 12-month period prior to Screening Visit 1.
  10. Negative urine pregnancy test for women of childbearing potential (WOCBP; after menarche) at Screening and Baseline.
  11. WOCBP (after menarche) must use either of the following methods of birth control, from Screening Visit 1 through the End of Study Visit: a. A highly effective form of birth control (confirmed by the investigator). Highly effective forms of birth control include: true sexual abstinence, a vasectomized sexual partner, Implanon, female sterilization by tubal occlusion, any effective intrauterine device (IUD), IUD/intrauterine system (IUS), Levonorgestrel IUS, or oral contraceptive. Or b. Two protocol acceptable methods of contraception in tandem. Women not of childbearing potential are defined as women who are either permanently sterilized (hysterectomy, bilateral oophorectomy, or bilateral salpingectomy) or who are postmenopausal. Women will be considered postmenopausal if they have been amenorrheic for ≥12 months prior to the planned date of the Baseline Visit without an alternative medical cause. The following age specific requirements apply: c. Women <50 years old will be considered postmenopausal if they have been amenorrheic for 12 months or more following cessation of exogenous hormonal treatment and follicle stimulating hormone levels in the postmenopausal range. d. Women ≥50 years old will be considered postmenopausal if they have been amenorrheic for 12 months or more following cessation of all exogenous hormonal treatment.

Exclusion criteria 29

  1. A participant who experiences a severe asthma exacerbation (defined as a deterioration of asthma that results in emergency treatment, hospitalization due to asthma, or treatment with systemic corticosteroids) at any time from 4 weeks prior to Screening Visit 1 up to and including the Baseline Visit. Participants who experience an asthma exacerbation during the Screening/Run-in Period may remain in Screening and proceed with study visits 14 days after they have completed their course of oral steroids or returned to their pre-Screening Visit maintenance dose of oral steroids and the investigator considers participant has returned to baseline status.
  2. Current diagnosis of diseases which may confound interpretation of this study’s findings such as allergic bronchopulmonary aspergillosis, eosinophilic granulomatosis with polyangiitis, eosinophilic gastrointestinal diseases, hypereosinophilic syndrome, or lung diseases (eg, chronic obstructive pulmonary disease, idiopathic pulmonary fibrosis).
  3. Respiratory infection: Upper or lower respiratory tract, sinus, or middle ear infection within the 4 weeks before Screening Visit 1.
  4. Treatment with a biologic investigational drug in the last 5 months prior to Screening Visit 1. Treatment with non-biologic investigational drugs in the previous 30 days or five-half-lives prior to Screening Visit 1, whichever is longer. Treatment with GSK3511294 (long-acting anti-interleukin [IL]-5) in the past 12 months.
  5. Treatment with any of the following monoclonal antibody therapies within 120 days prior to Baseline: benralizumab, dupilumab, mepolizumab, reslizumab, omalizumab, tezepelumab, or tralokinumab.
  6. Treatment with pramipexole (Mirapex®) within 30 days of Baseline.
  7. Treatment with selected drugs known to have a substantial risk of neutropenia in the past 30 days prior to Screening Visit 1 (see Appendix A).
  8. Bronchial thermoplasty procedure in the past 12 months prior to Screening Visit 1 or planned during the coming year.
  9. Weight <40 kg at Screening Visit 1.
  10. Current smoking within 12 months prior to Screening Visit 1 or a smoking history of >10 pack-years. Smoking includes tobacco, vaping, and/or marijuana use.
  11. Known or suspected alcohol or drug abuse.
  12. Uncontrolled severe hypertension: systolic blood pressure >180 mmHg or diastolic blood pressure >110 mmHg prior to the Baseline Visit despite anti-hypertensive therapy.
  13. History of malignancy that required surgery (excluding local and wide-local excision), radiation therapy and/or systemic therapy during the 5 years prior to the Baseline Visit.
  14. History of human immunodeficiency virus (HIV) infection or chronic infection with hepatitis B or C.
  15. A helminth parasitic infection diagnosed within 24 weeks prior to Screening Visit 1 that has not been treated with or has failed to respond to standard of care (SoC) therapy.
  16. Medical or other condition likely to interfere with participant’s ability to undergo study procedures, adhere to visit schedule, or comply with study requirements.
  17. Known or suspected noncompliance with medication.
  18. Unwillingness or inability to follow the procedures outlined in the protocol.
  19. Absolute neutrophil count <2.000x109/L at Screening Visit 1 or Screening Visit 2.
  20. Renal dysfunction, defined as an estimated glomerular filtration rate (eGFR) <60 mL/min/1.73m2 at Screening Visit 2 (using the Chronic Kidney Disease Epidemiology Collaboration [CKD-EPI] formula [Levey et al, 2009] for age ≥18 years at screening; using the Bedside Schwartz [Schwartz and Work, 2009] eGFR formula for age <18).
  21. Active liver disease defined as any known current infectious, neoplastic, or metabolic pathology of the liver or unexplained elevations in alanine aminotransferase (ALT), aspartate aminotransferase (AST), >3x the upper limit of normal (ULN), or total bilirubin >2x ULN at Screening Visit 2 confirmed by a repeat abnormal measurement of the relevant value(s), at least 1 week apart.
  22. History of New York Heart Association class IV heart failure or last known left ventricular ejection fraction <25%.
  23. History of major adverse cardiovascular event (MACE) within 3 months prior to the Baseline Visit.
  24. History of cardiac arrhythmia within 3 months prior to the Baseline Visit that is not controlled by medication or via ablation.
  25. History of long QT syndrome.
  26. Corrected QT interval by Fridericia (QTcF) interval >450 ms for males and >470 ms for females at Screening Visit 2 or QTcF ≥480 ms for participants with bundle branch block.
  27. Clinically important abnormalities in resting ECG that may interfere with the interpretation of QTcF interval changes at Screening Visit 2, including resting heart rate <45 beats per minute (bpm) or >100 bpm.
  28. Pregnant women or women breastfeeding.
  29. Males who are unwilling to use an acceptable method of birth control during the entire study period (ie, condom with spermicide).

Endpoints

Primary and secondary outcome measures (English text)

Primary endpoints 1

  1. Annualized rate of severe asthma exacerbations (AAER) over 52 weeks.

Secondary endpoints 3

  1. Pre-BD FEV1, absolute change from baseline, averaged across visits at Weeks 36, 44, and 52.
  2. Asthma Control Questionnaire-6 (ACQ-6), change from baseline, averaged across visits at Weeks 36, 44, and 52.
  3. Standardized version of the Asthma Quality of Life Questionnaire for 12 years and older (AQLQ+12), change from baseline to Week 52.

Investigational products

Investigational medicinal products (IMPs), comparators, placebo, auxiliary

Test 2

Dexpramipexole (KNS-760704)

PRD10251347 · Product

Active substance
Dexpramipexole Dihydrochloride Monohydrate
Substance synonyms
(6R)-4,5,6,7-tetrahydro-N6-propyl-2,6-benzothiazole-diamine dihydrochloride monohydrate
Pharmaceutical form
FILM-COATED TABLET
Route of administration
ORAL USE
Max daily dose
300 mg milligram(s)
Max total dose
105000 mg milligram(s)
Max treatment duration
52 Week(s)
Authorisation status
Not Authorised
MA holder
ARETEIA THERAPEUTICS
Paediatric formulation
No
Orphan designation
No

Dexpramipexole (KNS-760704)

PRD10251346 · Product

Active substance
Dexpramipexole Dihydrochloride Monohydrate
Substance synonyms
(6R)-4,5,6,7-tetrahydro-N6-propyl-2,6-benzothiazole-diamine dihydrochloride monohydrate
Pharmaceutical form
FILM-COATED TABLET
Route of administration
ORAL USE
Max daily dose
150 mg milligram(s)
Max total dose
54600 mg milligram(s)
Max treatment duration
52 Week(s)
Authorisation status
Not Authorised
MA holder
ARETEIA THERAPEUTICS
Paediatric formulation
No
Orphan designation
No

Placebo 1

Placebo

N/A · Product

Other product name
N/A
Pharmaceutical form
N/A
ATC code
N/A — N/A
Marketing authorisation
N/A
MA holder
N/A
MA country
Iceland
Paediatric formulation
No

Auxiliary 7

Ventolin 100 microgramos/inhalación suspensión para inhalación en envase a presión* (*) sin CFC

PRD391605 · Product

Active substance
Salbutamol Sulfate
Substance synonyms
Salbutamol hemisulfate, ALBUTEROL SULFATE, ALBUTEROL SULPHATE, SALBUTAMOL SULPHATE
Pharmaceutical form
PRESSURISED INHALATION, SUSPENSION
Route of administration
INHALATION USE
Max daily dose
1000 µg microgram(s)
Max total dose
425000 µg microgram(s)
Max treatment duration
425 Day(s)
Authorisation status
Authorised
ATC code
R03AC02 — SALBUTAMOL
Marketing authorisation
53.010
MA holder
GLAXOSMITHKLINE, S.A.
MA country
Spain
Paediatric formulation
No
Orphan designation
No
Modified vs. Marketing Authorisation
No

Ventolin 100 mikrogramų/išpurškime suslėgtoji įkvepiamoji suspensija

PRD390130 · Product

Active substance
Salbutamol Sulfate
Substance synonyms
Salbutamol hemisulfate, ALBUTEROL SULFATE, ALBUTEROL SULPHATE, SALBUTAMOL SULPHATE
Pharmaceutical form
PRESSURISED INHALATION, SUSPENSION
Route of administration
INHALATION USE
Max daily dose
1000 µg microgram(s)
Max total dose
425000 µg microgram(s)
Max treatment duration
425 Day(s)
Authorisation status
Authorised
ATC code
R03AC02 — SALBUTAMOL
Marketing authorisation
LT/1/94/1341/002
MA holder
GLAXOSMITHKLINE TRADING SERVICES LIMITED
MA country
Lithuania
Paediatric formulation
No
Orphan designation
No
Modified vs. Marketing Authorisation
No

Sultanol Dosier-Aerosol 100 Mikrogramm/Dosis Druckgasinhalation, Suspension

PRD378061 · Product

Active substance
Salbutamol Sulfate Ph. Eur.
Pharmaceutical form
PRESSURISED INHALATION, SUSPENSION
Route of administration
INHALATION USE
Max daily dose
1000 µg microgram(s)
Max total dose
425000 µg microgram(s)
Max treatment duration
425 Day(s)
Authorisation status
Authorised
ATC code
R03AC02 — SALBUTAMOL
Marketing authorisation
40393.00.00
MA holder
GLAXOSMITHKLINE GMBH & CO. KG
MA country
Germany
Paediatric formulation
No
Orphan designation
No
Modified vs. Marketing Authorisation
No

Novolizer Salbutamol Meda 100 Mikrogramm/Dosis Pulver zur Inhalation

PRD537300 · Product

Active substance
Salbutamol Sulfate
Substance synonyms
Salbutamol hemisulfate, ALBUTEROL SULFATE, ALBUTEROL SULPHATE, SALBUTAMOL SULPHATE
Pharmaceutical form
INHALATION POWDER
Route of administration
INHALATION USE
Max daily dose
1000 µg microgram(s)
Max total dose
425000 µg microgram(s)
Max treatment duration
425 Day(s)
Authorisation status
Authorised
ATC code
R03AC02 — SALBUTAMOL
Marketing authorisation
1-25976
MA holder
MYLAN ÖSTERREICH GMBH
MA country
Austria
Paediatric formulation
No
Orphan designation
No
Modified vs. Marketing Authorisation
No

Ventolin Evohaler túlnyomásos inhalációs szuszpenzió

PRD401111 · Product

Active substance
Salbutamol Sulfate
Substance synonyms
Salbutamol hemisulfate, ALBUTEROL SULFATE, ALBUTEROL SULPHATE, SALBUTAMOL SULPHATE
Pharmaceutical form
PRESSURISED INHALATION, SUSPENSION
Route of administration
INHALATION USE
Max daily dose
1000 µg microgram(s)
Max total dose
425000 µg microgram(s)
Max treatment duration
425 Day(s)
Authorisation status
Authorised
ATC code
R03AC02 — SALBUTAMOL
Marketing authorisation
OGYI-T-7232/01
MA holder
GLAXOSMITHKLINE TRADING SERVICES LIMITED
MA country
Hungary
Paediatric formulation
No
Orphan designation
No
Modified vs. Marketing Authorisation
No

Ventolin Inhaler N Suspenze k inhalaci v tlakovém obalu

PRD418497 · Product

Active substance
Salbutamol Sulfate
Pharmaceutical form
PRESSURISED INHALATION, SUSPENSION
Route of administration
INHALATION USE
Max daily dose
1000 µg microgram(s)
Max total dose
425000 µg microgram(s)
Max treatment duration
425 Day(s)
Authorisation status
Authorised
ATC code
R03AC02 — SALBUTAMOL
Marketing authorisation
14/869/99-C
MA holder
GLAXOSMITHKLINE (IRELAND) LIMITED
MA country
Czech Republic
Paediatric formulation
No
Orphan designation
No
Modified vs. Marketing Authorisation
No

Budesonide/Formoterol Teva Pharma B.V. 160 micrograms / 4.5 micrograms inhalation powder

PRD8003526 · Product

Active substance
Budesonide
Pharmaceutical form
INHALATION POWDER
Route of administration
INHALATION USE
Max daily dose
2400 µg microgram(s)
Max total dose
1020000 µg microgram(s)
Max treatment duration
425 Day(s)
Authorisation status
Authorised
ATC code
R03AK07 — FORMOTEROL AND OTHER DRUGS FOR OBSTRUCTIVE AIRWAY DISEASES
Marketing authorisation
EU/1/19/1403/002
MA holder
TEVA PHARMA B.V.
MA country
Liechtenstein
Paediatric formulation
No
Orphan designation
No
Modified vs. Marketing Authorisation
No

Sponsors and contacts

Sponsor organisations, regulatory contacts, third parties

Areteia Therapeutics Inc.

5 Total trials 3 Ended
Commercial
Sponsor organisation
Areteia Therapeutics Inc.
Address
1200 Morris Turnpike Suite 3005
City
Short Hills
Postcode
07078-2766
Country
United States

Scientific contact point

Organisation
Areteia Therapeutics Inc.
Contact name
Andrew Friedman

Public contact point

Organisation
Areteia Therapeutics Inc.
Contact name
Andrew Friedman

Third parties 14

OrganisationCity, countryDuties
Greenphire LLC
ORG-100041621
 King Of Prussia, United States Other
Quotient Sciences Philadelphia LLC
ORG-100018487
 Boothwyn, United States Code 14
GRCI Law Limited
ORL-000001021
 Ely, Cambridgeshire, United Kingdom Other
Merative US LP
ORG-100046293
 Ann Arbor, United States E-data capture
eResearchTechnology GmbH
ORG-100044103
 Estenfeld, Germany Other
Curia New York Inc.
ORG-100012294
 Rensselaer, United States Other
Almac
ORG-100013160
 Souderton, United States Code 14
Syneos Health France S.A.R.L.
ORG-100043413
 Biot, France Laboratory analysis
MEDPACE LABORATORIES
ORG-100042942
 Leuven, Belgium Laboratory analysis
SanaClis s.r.o.
ORG-100033651
 Bratislava, Slovakia Code 14
Yourway Transport Inc.
ORG-100046866
 Allentown, United States Code 14
Primevigilance USA Inc.
ORG-100047266
 Raleigh, United States Code 8
Worldwide Clinical Trials
ORG-100030991
 Grad Zagreb, Croatia On site monitoring, Code 10, Code 12, Code 13, Other, Code 2, Code 5, Data management, Code 8
WCG Clinical Inc.
ORG-100040730
 Princeton, United States Other

Locations

1 EU/EEA country · 6 investigational sites

By country

CountryMS statusPlanned subjectsSites
Czechia Not authorised 20 6
Rest of world
Australia, Turkey, South Africa, Lebanon, Chile, Israel, United Kingdom, Argentina, Taiwan, Korea, Republic of, United States, Peru, Mexico, Brazil
 834

Investigational sites

Czechia

6 sites · Not authorised
MediTrial s.r.o.
Plicní ambulance, Saldova 466/34, Karlin, Prague 8
University Hospital Olomouc
Klinikika plicních nemocí a tuberkulózy, Zdravotniku 248/7, 779 00, Olomouc
CEFISPIRO s.r.o.
Pneumologie, Terezínská 487/71, 410 02, Lovosice
Fakultni Nemocnice Brno
Klinika nemocí plicních a tuberkulózy, Jihlavska 340/20, Bohunice, Brno
Plicni Stredisko Teplice s.r.o.
Plicní ordinace, U Nadrazi 742/9, 415 01, Teplice
Plicní ordinace MUDr. Jaroslav Mareš
Plicní ordinace, 5.května 245, 38601, Strakonice

Application history

1 submissions — initial application plus substantial / non-substantial modifications

#TypeCodeSubmittedReference MSConclusionDecision date
1 INITIAL IN 2023-05-18 Not acceptable
2023-09-11
 2023-09-12

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