NCT03748199

Brief Summary

"This is a randomised, double-blind, placebo-controlled multi-centre study to investigate safety and tolerability and to provide pharmacokinetic and pharmacodynamics information of orally inhaled multiple doses (80 mg, 160 mg or 320 mg) of the nebulised neutrophil elastase inhibitor POL6014 in patients with Cystic Fibrosis. The controlled inhalation will occur via the eFlow® nebuliser system (manufacturer: PARI Pharma GmbH, Germany)".

Trial Health

87
On Track

Trial Health Score

Automated assessment based on enrollment pace, timeline, and geographic reach

Enrollment
32

participants targeted

Target at P50-P75 for phase_1

Timeline
Completed

Started Nov 2018

Typical duration for phase_1

Geographic Reach
1 country

4 active sites

Status
completed

Health score is calculated from publicly available data and should be used for screening purposes only.

Trial Relationships

Click on a node to explore related trials.

Study Timeline

Key milestones and dates

First Submitted

Initial submission to the registry

November 5, 2018

Completed
3 days until next milestone

Study Start

First participant enrolled

November 8, 2018

Completed
12 days until next milestone

First Posted

Study publicly available on registry

November 20, 2018

Completed
2.1 years until next milestone

Primary Completion

Last participant's last visit for primary outcome

December 30, 2020

Completed
Same day until next milestone

Study Completion

Last participant's last visit for all outcomes

December 30, 2020

Completed
Last Updated

September 28, 2021

Status Verified

March 1, 2021

Enrollment Period

2.1 years

First QC Date

November 5, 2018

Last Update Submit

September 22, 2021

Conditions

Cystic Fibrosis

Keywords

CFcystic fibrosisPOL6014neutrophil elastase inhibitoranti-inflammatory

Outcome Measures

Primary Outcomes (10)

  • Safety measured by proportion of patients who experience potential clinically significant changes in physical examinations

    Baseline through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by number of patients with changes in laboratory assessments (clinical chemistry, haematology, urinanalysis)

    Baseline through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by number of patients with changes in vital signs (blood pressure, pulse, respiratory rate and body temperature)

    Baseline and pre-dose through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by number of patients with changes in ECG parameters (heart rythm, ventricular rate, PR interval, QRS duration, Qt and QTc)

    Baseline and pre-dose through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by occurrence and severity of adverse events

    Baseline through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by proportion of subjects who experience local irritation of the nose or pharynx by visual inspection

    Baseline through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by proportion of patients who experience bronchospasm

    Baseline through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by changes in lung function parameters (FEV1, FVC)

    Baseline and pre-dose through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Safety measured by changes in oxygen saturation in peripheral blood as measured by pulse oximetry

    Baseline through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

  • Tolerability assessed by the number of patients who discontinue the study treatment prematurely due to Adverse Events

    Baseline through end of treatment (up to 15 days for cohorts 1A/2A/2B, up to 28 days for cohort C)

Secondary Outcomes (1)

  • Pharmacokinetics (PK) for POL6014 and metabolites in plasma, sputum and urine

    At defined timepoints (Day1, Day 2, Day 8, Day 14, Day 15, Day 16)

Study Arms (2)

POL6014

EXPERIMENTAL

multiple ascending doses: 80, 160 and 40 mg once or twice daily

Drug: POL6014

Placebo

PLACEBO COMPARATOR

Placebo will be administered orally at a dose and frequency matched to POL6014

Drug: Placebo

Interventions

POL6014DRUG

DL1 80 mg cohorts 1A and 1B (80 mg QD and 40 mg BID) DL2 160 mg cohorts 2A and 2B (160 mg QD and 80 mg BID) DL3 40 mg QD cohort C DL = dose Level QD= quaque die (once daily) BID= bis in die (twice daily)

POL6014
PlaceboDRUG

Placebo will be administered orally at a dose and frequency matched to POL6014

Placebo

Eligibility Criteria

Age18 Years - 55 Years
Sexall
Healthy VolunteersNo
Age GroupsAdult (18-64)

You may qualify if:

  • Patient has given written informed consent to participation in the trial prior to their enrolment and any trial-related procedure.
  • Male patients or female patients of non-childbearing potential, aged 18 to 55 years, inclusive. Women of non-childbearing potential are defined as those who have no uterus, or ligation of the fallopian tubes, or permanent cessation of ovarian function due to ovarian failure or surgical removal of the ovaries. Documentation of surgical procedure is required for patients who have had a hysterectomy or tubal ligation.
  • Men must agree to practice contraception from start of study medication up to 90 days after the last dose of the study medication.
  • Patient with a diagnosis of CF documented by a compatible clinical or radiographic presentation and laboratory criteria, more specifically, sweat or genetic testing (i.e., presence of the most common genetic defect ΔF 508 or any other mutation that can produce CF).
  • Patient should confirm to produce frequently spontaneous sputum with a frequency of over 3 expectorates per day. Patient should be capable of producing a spontaneous sputum sample at screening (within a time range of approx. 3h during the screening visit).
  • Except for CF and CF-related diseases, no other significant disease as assessed by a screening examination including medical history, physical examination, vital signs, ECG assessment, pulmonary function testing (PFT), and clinical laboratory results. Deviations of clinical laboratory results can be accepted if they are in accordance with the diagnosis of CF and CF-related diseases, supposed they do not indicate a clinical state that is expected to constitute a significant additional risk.
  • Patient must have an FEV1 ≥ 40% of predicted value at screening.
  • Body mass index (BMI) between 16.5 and 30 (both inclusive).
  • Non-smoker or ex-smoker who has stopped smoking for at least one (1) year prior to the Screening Visit.
  • Patient should be willing to refrain from caffeine- or theophylline-containing products within 24 h prior to a clinic visit for a full PK profile.
  • Ability to inhale in an appropriate manner (Patients will be trained to inhale from the eFlow® nebuliser device with a commercially available saline solution at the Screening Visit once informed consent has been obtained).
  • For patients with routine courses of inhaled antibiotics, patients should agree to start routine course of inhaled antibiotic cycle on the same day or not earlier than 3 days before IMP administration.

You may not qualify if:

  • Patient with unstable lung disease, as defined by a change in treatment regimen during the preceding two (2) weeks, or a significant new finding on chest radiography (such as, but not limited to, pneumothorax, lobar/segmental collapse or consolidation), or in the opinion of the investigator, patient with a decline in pulmonary status within the last 12 months not considered a part of the usual, chronic progression of CF lung disease. Routine cyclic antibiotic treatment regimens including "off/on" cycles are not considered to be changes to treatment regimens.
  • Patient has had an exacerbation of respiratory symptoms within the past four (4) weeks before screening/randomization that required initiation of a new or altered respiratory therapy, and, in the opinion of the investigator, the patient has not returned to a stable level of health
  • Patient with a history of lung transplantation.
  • Patient with a history of clinically significant renal, hepatic, gastrointestinal,cardiovascular and particularly respiratory disease (excluding CF and CF-related disease).
  • Patient with active gastrointestinal ulcer, history of intracranial bleedings, injuries and other bleedings.
  • Patient, as per assessment of the investigator, with severe hepatic impairment (e.g. laboratory values (ALT, AST \> 3 x ULN and total bilirubin \> 1.5 x ULN) or Child-Pugh-Class C could be indicative of such condition).
  • ECG abnormalities of clinical relevance (e.g., QTc according to Bazett's formula ≥440 ms, PR \>200 ms, or QRS ≥120 ms).
  • Patient with a resting heart rate in supine position \<50 bpm, systolic blood pressure \<100 mmHg or \>140 mmHg, diastolic blood pressure \<60 mmHg or \>90 mmHg.
  • Proneness to orthostatic dysregulation, fainting, or blackouts.
  • Diagnosis of a tricuspid insufficiency in combination with a mean pulmonary arterial pressure (mPAP) \> 25 mmHg, measured by Doppler echography, or, if no tricuspid insufficiency is detectable, any echocardiographic or clinical signs of severe pulmonary heart disease (cor pulmonale) or depending congestive heart failure.
  • History or presence of any malignancy.
  • Positive results in any of the following virology tests: human immunodeficiency virus (HIV) antibodies and antigen, Anti-hepatitis B-core antibody, hepatitis B surface antigen (HbsAg) and anti-hepatitis C virus antibody.
  • Known local or systemic hypersensitivity to any aerosol, medication or food that led to admission to an emergency room.
  • Participation in another clinical study with any investigational medicinal product (IMP) or device, before randomisation, within an interval of 5 half-lives (minimum 4 weeks) from the last use of that investigational drug.
  • Blood or plasma donation of more than 500 mL during the previous month before randomisation, as declared by the patient.
  • +2 more criteria

Contact the study team to confirm eligibility.

Sponsors & Collaborators

Study Sites (4)

Charité - Uniklinik Berlin, Klinik für Pädiatrie,Pneumologie, Immunologie, Erwachsenene-Mucoviszidose

Berlin, 13353, Germany

Location

Ruhrlandklinik Westdeutsches Lungenzentrum

Essen, 45239, Germany

Location

IKF Pneumologie GmbH & Co. KG, Institut für klinische Forschung Pneumologie

Frankfurt, 60596, Germany

Location

Inamed GmbH, clinical unit

Gauting, 82131, Germany

Location

MeSH Terms

Conditions

Cystic Fibrosis

Interventions

lonodelestat

Condition Hierarchy (Ancestors)

Pancreatic DiseasesDigestive System DiseasesLung DiseasesRespiratory Tract DiseasesGenetic Diseases, InbornCongenital, Hereditary, and Neonatal Diseases and AbnormalitiesInfant, Newborn, Diseases

Study Design

Study Type
interventional
Phase
phase 1
Allocation
RANDOMIZED
Masking
DOUBLE
Who Masked
PARTICIPANT, INVESTIGATOR
Purpose
TREATMENT
Intervention Model
SEQUENTIAL
Sponsor Type
INDUSTRY
Responsible Party
SPONSOR

Study Record Dates

First Submitted

November 5, 2018

First Posted

November 20, 2018

Study Start

November 8, 2018

Primary Completion

December 30, 2020

Study Completion

December 30, 2020

Last Updated

September 28, 2021

Record last verified: 2021-03

Locations

DE(4)