Phase 3
Completed N=83
A Study to Evaluate the Pharmacokinetics, Safety, and Tolerability of VX-661/Ivacaftor in Pediatric Subjects With Cystic Fibrosis (CF)
Source: ClinicalTrials.gov NCT02953314 ↗Enrolled (actual)
83
Serious AEs
7.2%
Results posted
Dec 2019
Primary outcomePrimary: Part A: Maximum Observed Concentration (Cmax) of TEZ and IVA — 6630; 4310; 6300; 5340 nanogram per milliliter (ng/mL)
◆ Published Evidence
Established
55citations · ~8 / year
A phase 3 study of tezacaftor in combination with ivacaftor in children aged 6 through 11 years with cystic fibrosis.
Summary
This is a Phase 3, 2-part (Part A and Part B), open label, multicenter study evaluating the pharmacokinetic (PK), safety, and tolerability of multiple doses of tezacaftor (TEZ) in combination with ivacaftor (IVA) in subjects 6 through 11 years of age with CF who are homozygous or heterozygous for the F508del- CF transmembrane conductance regulator protein (CFTR) mutation.
Linked Publications
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A phase 3 study of tezacaftor in combination with ivacaftor in children aged 6 through 11 years with cystic fibrosis.
Outcome Measures
| Outcome | Result | p-value |
|---|---|---|
| PRIMARY Part A: Maximum Observed Concentration (Cmax) of TEZ and IVA |
6630; 4310; 6300; 5340; 656; 1010 | — |
| PRIMARY Part A: Area Under the Concentration Versus Time Curve During Dosing Interval (AUCtau) of TEZ and IVA |
54300; 41600; 66500; 71600; 5050; 12400 | — |
| PRIMARY Part B: Number of Participants With Treatment-Emergent Adverse Events (AEs) and Serious Adverse Events (SAEs) |
65; 6 | — |
| SECONDARY Part A: Cmax of TEZ Metabolites (M1-TEZ, M2-TEZ) and IVA Metabolites (M1-IVA, M6-IVA) |
1720; 1530; 8360; 5930; 1130; 922 | — |
| SECONDARY Part A: AUCtau of TEZ Metabolites (M1-TEZ, M2-TEZ) and IVA Metabolites (M1-IVA, M6-IVA) |
36500; 27400; 160000; 121000; 14200; 11100 | — |
| SECONDARY Part A: Number of Participants With AEs and SAEs |
12; 0 | — |
| SECONDARY Part B: Cmax of TEZ, TEZ Metabolites (M1-TEZ, M2-TEZ), IVA, and IVA Metabolites (M1-IVA, M6-IVA) |
4800; 5870; 5310; 5440; 4170; 5210 | — |
| SECONDARY Part B: AUCtau of TEZ, TEZ Metabolites (M1-TEZ, M2-TEZ), IVA, and IVA Metabolites (M1-IVA, M6-IVA ) |
50300; 60900; 104000; 100000; 88400; 93600 | — |
| SECONDARY Part B: Absolute Change in Percent Predicted Forced Expiratory Volume in 1 Second (ppFEV1) |
0.9 | — |
| SECONDARY Part B: Relative Change in ppFEV1 |
1.4 | — |
| SECONDARY Part B: Absolute Change in Weight |
1.7 | — |
| SECONDARY Part B: Absolute Change in Weight-for-age Z-Score |
0.00 | — |
| SECONDARY Part B: Absolute Change in Height |
2.7 | — |
| SECONDARY Part B: Absolute Change in Height-for-age z-Score |
0.00 | — |
| SECONDARY Part B: Absolute Change in Body Mass Index (BMI) |
0.23 | — |
| SECONDARY Part B: Absolute Change in BMI-for-age z-Score |
-0.03 | — |
| SECONDARY Part B: Absolute Change in Sweat Chloride |
-14.5 | — |
| SECONDARY Part B: Absolute Change in Sweat Chloride |
-14.5 | — |
| SECONDARY Part B: Absolute Change in Cystic Fibrosis Questionnaire-Revised (CFQ-R) Respiratory Domain Score |
3.4 | — |
Eligibility Criteria
Inclusion Criteria
- Subjects who weigh ≥15 kg without shoes at the Screening Visit.
- All genotypes as specified by the study protocol are eligible in Part A.
- The following genotypes are eligible in Part B:
- homozygous for the F508del CFTR mutation
- heterozygous for the F508del CFTR mutation and with a second allele with a CFTR mutation predicted to have residual function.
- heterozygous for the F508del CFTR mutation and with a second CFTR allele with a gating defect that is clinically demonstrated to be ivacaftor responsive
- Subjects with a confirmed diagnosis of CF defined as a sweat chloride value ≥60 mmol/L or chronic sinopulmonary and/or gastrointestinal disease consistent with a diagnosis of CF. Subjects who are homozygous for the F508del-CFTR mutation must have a sweat chloride value ≥60 mmol/L.
- Subjects with ppFEV1 of ≥40 percentage points at the Screening Visit
- Subjects with stable CF disease as deemed by the investigator at the Screening Visit.
- Subjects who are willing to remain on their stable CF medication regimen through Day 14 (Part A) or through Week 24 (Part B) or, if applicable, through the Safety Follow up Visit.
- Subjects who are able to swallow tablets.
- Female subjects of childbearing potential must have a negative serum pregnancy test at the Screening Visit and a negative urine pregnancy test at the Day 1 Visit before receiving the first dose of study drug.
- Subjects of childbearing potential who are sexually active must meet the contraception requirements
Exclusion Criteria
- History of any comorbidity reviewed at the Screening Visit that, in the opinion of the investigator, might confound the results of the study or pose an additional risk in administering study drug to the subject.
- Any clinically significant laboratory abnormalities at the Screening Visit that would interfere with the study assessments or pose an undue risk for the subject.
- An acute upper or lower respiratory infection, pulmonary exacerbation, or changes in therapy for pulmonary disease within 28 days before Day 1
- Colonization with organisms associated with a more rapid decline in pulmonary status.
- A standard 12 lead ECG demonstrating QTc >450 msec at the Screening Visit.
- History of solid organ or hematological transplantation at the Screening Visit.
- Ongoing or prior participation in an investigational drug study or use of commercially available CFTR modulator (except physician-prescribed Kalydeco for approved indications) within 30 days of screening.
- Use of restricted medication or food within a specified duration before the Screening Visit or first dose of study drug and/or unwillingness to maintain the restrictions.
- History or evidence of cataract, lens opacity, Y-suture, or lamellar rings determined to be clinically significant by the ophthalmologist during the ophthalmologic examination at the Screening Visit.
- Pregnant and nursing females.
Data sourced from ClinicalTrials.gov (NCT02953314) and the linked publication. Outcome figures and adverse-event rates are extracted automatically from the registry's posted results and are provided for clinician reference, not as a substitute for the primary publication. Informational only — not medical advice.