Safety Study of Ivacaftor in Subjects With Cystic Fibrosis

Phase 2

Completed

• Conditions: Cystic Fibrosis
• Interventions: Drug: Ivacaftor 75 mg/150 mg; Drug: Ivacaftor 150 mg or 250 mg; Drug: Ivacaftor 25 mg/75 mg; Drug: Placebo

• Registration Number: NCT00457821
• Lead Sponsor: Vertex Pharmaceuticals Incorporated

Brief Summary

The purpose of this study was to evaluate the safety and tolerability of ivacaftor in patients with cystic fibrosis (CF) who were aged 18 years or older and have a G551D mutation in the cystic fibrosis transmembrane conductance regulator (CFTR) gene. Ivacaftor is a potent and selective CFTR potentiator of wild-type, G551D, F508del, and R117H forms of human CFTR protein. Potentiators are pharmacological agents that increase the chloride ion transport properties of the channel in the presence of cyclic AMP-dependent protein kinase A (PKA) activation.

Detailed Description

This was a double-blind, placebo-controlled, cross-over, multiple dose study of up to 28 days of dosing, in subjects with cystic fibrosis (CF) who have a G551D-CTFR gene mutation. Enrollment of 39 subjects occurred at 15 centers in the US, Canada, and Germany.

The study was conducted in 2 parts:

* Part 1 consisted of Group A and Group B. Subjects in Group A (10 subjects) were randomized to receive 25 mg of ivacaftor every 12 hours \[q12h\] (4 subjects), 75 mg of ivacaftor q12h (4 subjects), or placebo (2 subjects) for 14 days. Following a 7- to 28-day washout period, subjects who received active study drug crossed over to the alternate dose strength of ivacaftor for an additional 14 days. Placebo subjects continued to receive placebo for an additional 14 days. Subjects in Group B (10 subjects) were randomized to receive 75 mg of ivacaftor q12h (4 subjects), 150 mg of ivacaftor q12h (4 subjects), or placebo (2 subjects) for 14 days. Following a 7- to 28-day washout period, the subjects who received active study drug crossed over to the alternate dose strength of ivacaftor for an additional 14 days. Placebo subjects continued to receive placebo for an additional 14 days.

* Part 2 consisted of Group C; these subjects did not participate in Part 1. Subjects were randomized to receive 150 mg of ivacaftor q12h (7 subjects), 250 mg of ivacaftor q12h (7 subjects), or placebo (4 subjects) for a total of 28 days. Ivacaftor doses studied in Part 2 were selected following an interim pharmacokinetic/pharmacodynamic (PK/PD) and statistical analyses of data from Part 1. The 2 doses selected for Part 2 were anticipated to enable better definition of the optimal therapeutic dose.

Study Timeline

• Study First Submitted: 2007-04-05
• Study First Submitted QC: 2007-04-05
• Study First Posted: 2007-04-09
• Study Start: 2007-05
• Primary Completion: 2008-08
• Study Completion: 2008-08
• Disposition First Submitted: 2010-08-31
• Disposition First Submitted QC: 2010-08-31
• Disposition First Posted: 2010-09-06
• Results First Submitted: 2012-02-27
• Status Verified: 2012-10
• Results First Submitted QC: 2012-10-03
• Last Update Submitted: 2012-10-03
• Results First Posted: 2012-10-05
• Last Update Posted: 2012-10-05

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 39

Inclusion Criteria

• Weighing at least 40 kg
• Confirmed diagnosis of cystic fibrosis (CF) and G551D mutation in at least 1 allele
• Forced expiratory volume in 1 second (FEV1) of at least 40% of predicted normal for age, gender, and height
• Willing to remain on stable medication regimen for the duration of study participation
• No significant clinical laboratory abnormalities, not pregnant, and willing to use at least 2 highly effective birth control methods during Part 1 and 1 highly effective birth control method during Part 2 of the study
• No clinically significant abnormalities that would have interfered with the study assessments, as judged by the investigator

Exclusion Criteria

• History of any illness or condition that might confound the results of the study or pose an additional risk in administering study drug to the subject
• Ongoing acute respiratory infection, pulmonary exacerbation, or changes in therapy for pulmonary disease within 14 days of Day 1 of the study
• History of alcohol, medication or illicit drug abuse within one year prior to Day 1
• Abnormal liver function ≥ 3x the upper limit of normal
• History of abnormal renal function (creatinine clearance < 50 mL/min using Cockcroft-Gault equation)
• History of solid organ or hematological transplantation
• Pregnant or breast-feeding (for women)
• Ongoing participation in another therapeutic clinical trial, or prior participation in an investigational drug study without appropriate washout
• Concomitant use of any inhibitors or inducers of cytochrome P450 3A4 (CYP3A4)

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: CROSSOVER

Arm && Interventions

Group	Intervention	Description
Ivacaftor Group B	Ivacaftor 75 mg/150 mg	Subjects in Part 1 who first received 75 mg or 150 mg of ivacaftor q12h for 14 days then crossed over to receive the alternate dose for another 14 days.
Ivacaftor Group C	Ivacaftor 150 mg or 250 mg	Subjects in Part 2 who received 150 mg or 250 mg of ivacaftor q12h for 28 days.
Ivacaftor Group A	Ivacaftor 25 mg/75 mg	Subjects in Part 1 who first received 25 mg or 75 mg of ivacaftor every 12 hours (q12h) for 14 days, then crossed over to receive the alternate dose for another 14 days.
Placebo	Placebo	Subjects who received placebo in Part 1 and subjects who received placebo in Part 2.

Primary Outcome Measures

Name	Time	Method
Number of Subjects With Adverse Events (Combined Part 1 and Part 2)	Baseline to Follow-up	Adverse event data were collected up to the follow-up visit (5 to 9 days after last dose of study drug). Serious adverse events that were ongoing at the follow-up visit were followed until the event resolved, returned to baseline, or was determined to be a stable or chronic condition.
Number of Adverse Events (Combined Part 1 and Part 2)	Baseline to Follow-up	Adverse event data were collected up to the follow-up visit (5 to 9 days after last dose of study drug). Serious adverse events that were ongoing at the follow-up visit were followed until the event resolved, returned to baseline, or was determined to be a stable or chronic condition.

Secondary Outcome Measures

Name	Time	Method
Change From Baseline in Nasal Potential Difference (Combined Part 1 and Part 2)	14 days and 28 days	The transepithelial nasal potential difference (NPD) is a direct measure of transepithelial ion transport. NPD under conditions of zero chloride concentration perfusion solution in the presence of isoproterenol was of primary interest.
Change From Baseline in Percent Predicted Forced Expiratory Volume in 1 Second [FEV1] (Combined Part 1 and Part 2)	14 days and 28 days	Spirometry is a standardized assessment to evaluate lung function that is the most widely used endpoint in cystic fibrosis studies.; Relative change reflects the percent change from the baseline values \[100% \* (X-Y)/Y\], where X and Y are post-baseline and baseline values, respectively.
Change From Baseline in the Cystic Fibrosis Questionnaire-Revised (CFQ-R) Score (Part 2 Only)(Respiratory Domain Score)	14 days and 28 days	The CFQ-R is a health-related quality of life measure for subjects with cystic fibrosis. Each domain is scored from 0 (worst) to 100 (best). A difference of at least 4 points in the respiratory domain score of the CFQ-R is considered a minimal clinically important difference (MCID).
Change From Baseline in Maximum Sweat Chloride Concentration (Combined Part 1 and Part 2)	14 days and 28 days	The sweat chloride (quantitative pilocarpine iontophoresis) test is a standard diagnostic tool for cystic fibrosis (CF), serving as an indicator of cystic fibrosis transmembrane conductance regulator (CFTR) activity.

Trial Locations

Locations (15)

Johns Hopkins Hospital; 🇺🇸 Baltimore, Maryland, United States

The Children's Hospital; 🇺🇸 Aurora, Colorado, United States

Stanford University Medical Center; 🇺🇸 Palo Alto, California, United States

University of Pittsburgh; 🇺🇸 Pittsburgh, Pennsylvania, United States

Pulmonary and Critical Care Medicine, Massachusetts General Hospital; 🇺🇸 Boston, Massachusetts, United States

Division of Pulmonary, Allergy and Critical Care Medicine, University of Minnesota; 🇺🇸 Minneapolis, Minnesota, United States

The Children's Hospital of Philadelphia; 🇺🇸 Philadelphia, Pennsylvania, United States

University of Alabama Hospital; 🇺🇸 Birmingham, Alabama, United States

Division of Gastroenterology, Hepatology and Nutrition, The Hospital for Sick Children; 🇨🇦 Toronto, Ontario, Canada

Cystic Fibrosis Pulmonary Research and Treatment Center, University of North Carolina at Chapel Hill; 🇺🇸 Chapel Hill, North Carolina, United States

Children's Hospital of Boston; 🇺🇸 Boston, Massachusetts, United States

CF Clinic, Pediatric Pulmonology and Neonatology, Medical School of Hannover; 🇩🇪 Strasse, Hannover, Germany

Pulmonary Critical Care, University of Washington; 🇺🇸 Seattle, Washington, United States

Rainbow Babies and Children's Hospital; 🇺🇸 Cleveland, Ohio, United States

Roy J. and Lucille A. Carver College of Medicine, The University of Iowa; 🇺🇸 Iowa City, Iowa, United States