Trientine Tetrahydrochloride (TETA 4HCL) for the Treatment of Wilson's Disease
Status: | Recruiting |
---|---|
Healthy: | No |
Age Range: | 18 - 75 |
Updated: | 1/27/2019 |
Start Date: | June 4, 2018 |
End Date: | July 2021 |
Contact: | Deirdre Kraimer |
Email: | deirdre@gmp-o.com |
Phone: | 860-910-5819 |
CHELATE STUDY: Trientine Tetrahydrochloride (TETA 4HCL) for the Treatment of Wilson's Disease
This is a multicenter, randomized, open-label study with an active standard-of-care
comparator (penicillamine)
comparator (penicillamine)
This is a multicenter, randomized, open label study with an active standard-of-care
comparator.
Stable patients who are already considered to be stable on their standard-of-care
penicillamine chelation therapy for at least 1 year will enroll in the study and enter a
12-week Penicillamine Baseline Period comprising of 1 month (4 weeks) run-in period followed
by a 2 month (8 weeks) evaluation period. During this time all patients will continue to take
their current penicillamine under study conditions. At the end of the Penicillamine Baseline
Period, patients who fulfill the protocol definition of being adequately controlled and
tolerating penicillamine will be randomized in a 1:1 ratio to receive either TETA 4HCl or to
continue to receive penicillamine. There is then a 24-week Post-randomization Phase
comprising of a 1 month (4 weeks) run-in period for both treatment arms and a 5 month (20
weeks) evaluation period.
Patients who successfully complete the 24-week Post-randomization Phase of the study will
have the opportunity to enter an 18 month (72 weeks) Extension Phase. Initially they continue
to receive their allocated TETA 4HCl or penicillamine for a further 24 weeks (i.e., up to
Week 60 of the study). Thereafter all patients will receive TETA 4HCl for 48 weeks (i.e.,
between Week 60 and Week 108). Study clinic visits occur every 6 months (24 weeks) for all
patients (i.e., at Weeks 60, 84 and 108).
comparator.
Stable patients who are already considered to be stable on their standard-of-care
penicillamine chelation therapy for at least 1 year will enroll in the study and enter a
12-week Penicillamine Baseline Period comprising of 1 month (4 weeks) run-in period followed
by a 2 month (8 weeks) evaluation period. During this time all patients will continue to take
their current penicillamine under study conditions. At the end of the Penicillamine Baseline
Period, patients who fulfill the protocol definition of being adequately controlled and
tolerating penicillamine will be randomized in a 1:1 ratio to receive either TETA 4HCl or to
continue to receive penicillamine. There is then a 24-week Post-randomization Phase
comprising of a 1 month (4 weeks) run-in period for both treatment arms and a 5 month (20
weeks) evaluation period.
Patients who successfully complete the 24-week Post-randomization Phase of the study will
have the opportunity to enter an 18 month (72 weeks) Extension Phase. Initially they continue
to receive their allocated TETA 4HCl or penicillamine for a further 24 weeks (i.e., up to
Week 60 of the study). Thereafter all patients will receive TETA 4HCl for 48 weeks (i.e.,
between Week 60 and Week 108). Study clinic visits occur every 6 months (24 weeks) for all
patients (i.e., at Weeks 60, 84 and 108).
Inclusion Criteria:
1. Patient is able to provide, and has provided, written informed consent
2. Written documentation has been obtained in accordance with the relevant country and
local privacy requirements, where applicable, including: For US sites: Authorization
for Use and Release of Health Research Study Information and for EU sites: Data
Protection Consent
3. Male or female, aged ≥ 18 and ≤ 75 years of age at time of consent
4. Patient has a diagnosis of Wilson's disease, as defined by a prior or current Leipzig
score of ≥ 4
5. Patient's Wilson's disease is clinically stable, in the opinion of the investigator,
and being treated with penicillamine for at least 1 year (52 weeks) prior to the
screening/enrolment visit
6. Patient is on a stable dose and regimen of penicillamine for at least 4 months (16
weeks) prior to the screening/enrolment visit (other prescribed treatments for
Wilson's disease not permitted during this study)
7. No anticipated need that patient will require additional pharmacological therapies
other than study medication, including prescribed zinc therapy, for the management of
copper levels during the study
8. Patient must be willing to maintain stable diet throughout the study, and avoid foods
with high copper content, including the Penicillamine Baseline Period
9. Patient considered suitable to receive therapy with both TETA 4HCl and penicillamine
administered twice a day
10. Negative central laboratory tests for HIV and viral hepatitis (results will be
available after start of run-in period)
11. For female patients of childbearing potential, negative urine pregnancy test (at
screening/enrolment visit and prior to randomization)
12. For females of childbearing potential, use of a reliable form of contraceptive
13. Patient is considered as able to complete study requirements and attend the study
visits, in the opinion of the investigator
Additional inclusion criteria following receipt of Screening laboratory results
14. Patient is adequately controlled and tolerating penicillamine therapy as defined by
fulfilment of all of the following: a. Serum non-ceruloplasmin bound copper (NCC)
level between ≥ 25 and ≤ 150 μg/L* b. 24-hour urinary copper excretion of between ≥
100 and ≤ 900 μg/24 hours* c. Alanine transaminase (ALT) < 2 times upper limit of
normal* d. No other laboratory or clinical findings that would prevent continuation of
maintenance therapy, in the opinion of the investigator
* Based on results from screening/enrolment visit samples for which can be taken
within ± 7 days of visit. Result should be within the assay limits of quantification
for the sample. The ranges in μmol of copper are 0.40 to 2.38 μmol/L for NCC and 1.59
to 14.29 for 24-hour urinary copper excretion (using division by 63 of value in μg per
Walshe, 2011). In the event that one or more of the above lab values fall outside the
specified range, it can be repeated, including at the Week 4 and Week 8 visits.
Additional inclusion criteria at Week 12 visit (end of Penicillamine Baseline Period)
and prior to randomization
15. Patient is adequately controlled and tolerating penicillamine therapy as defined by
fulfilment of all of the following criteria:
1. Serum non-ceruloplasmin bound copper (NCC) level between ≥ 25 and ≤ 150 μg/L*
2. 24-hour urinary copper excretion of between ≥ 100 and ≤ 900 μg/24 hours**
3. Alanine transaminase (ALT) < 2 times upper limit of normal*
4. No other laboratory or clinical findings that would prevent continuation of
maintenance therapy, in the opinion of the investigator
- Based on lab values from Week 8 visit; ** Based on lab value from Week 4
visit as routinely not performed at Week 8 visit, however can also be based
on value at Week 8 visit if a repeat (unscheduled) urinary copper excretion
was performed at this visit. Result should be within the assay limits of
quantification for the sample. The ranges in μmol of copper are 0.40 to 2.38
μmol/L for NCC and 1.59 to 14.29 for 24-hour urinary copper excretion (using
division by 63 of value in μg per Walshe, 2011). In the event that one or
more of the above lab values fall outside the specified range, it can be
repeated. The repeat value(s) must be available prior to randomization at
Week 12 and, if within specified range, the patient can continue to
randomization. If a patient fails this additional criterion at the end of
the Penicillamine Baseline Period, the patient can return to the start of
the run-in period i.e. Day 1 (but only once). A negative urinary pregnancy
test is also required prior to randomization for females of childbearing
potential.
Exclusion Criteria:
1. Patient is in 'de-coppering' phase of treatment for Wilson's disease, in the opinion
of the investigator
2. Patient evidence of uncontrolled liver disease, including but not limited to:
1. Modified Nazer score of > 4 (result may not be available until after start of run
in period since based on lab results*)
2. decompensated cirrhosis
3. acute hemolytic anemia
4. acute hepatitis
5. hepatic malignancy
6. evidence of acute liver failure
3. Cause of patient's liver disease is due to another condition, in the investigator's
opinion
4. Patient has severe anemia defined as hemoglobin of ≤ 9 g/dL (result will be available
after start of run-in period*)
5. Patient has experienced a gastrointestinal bleed within 6 months (24 weeks) prior to
screening/enrolment visit
6. Patient has renal impairment defined as creatinine clearance of ≤ 30 mL/min (result
may not be available until after start of run-in period*), or patient has nephritis or
nephrotic syndrome, in the opinion of the investigator
7. Patient has neurological disease that prevents swallowing of study medication (e.g.,
requires a nasogastric feeding tube) or requires intensive in-patient medical care
8. Patient is currently taking medication containing trientine for management of Wilson's
disease or has taken it within 4 months (16 weeks) of screening/enrolment visit
9. Patient is currently receiving prescribed zinc therapy for management of Wilson's
disease or has taken it within 4 months (16 weeks) of screening/enrolment visit
10. Patient is taking any of the following concomitant therapies: gold therapy,
antimalarial therapy, cytotoxic drugs, oxyphenbutazone, phenyl butazone
11. Patient has a known intolerance, allergy or sensitivity to penicillamine (that is
uncontrolled) or to TETA 4HCl, including any component of the study medication
12. For female patients of childbearing potential, planning a pregnancy during study
period or currently nursing
13. For female patients of childbearing potential, unable or unwilling to use a reliable
form of contraceptive throughout the study
14. Patient is currently participating in another therapeutic study, or has previously
participated in a therapeutic study within 30 days of screening/enrolment visit (or
longer, if local requirements specify this)
15. Patient has any condition or in any situation which, in the investigator's opinion,
puts the patient at significant risk, could confound study results, or may interfere
significantly with the patient's participation in the study
We found this trial at
2
sites
Leuven,
Principal Investigator: David Cassiman, MD
Phone: 32 16 34 46 49
Click here to add this to my saved trials
333 Cedar St
New Haven, Connecticut 06504
New Haven, Connecticut 06504
(203) 432-4771
Phone: 203-785-2480
Yale University School of Medicine Founded in 1810, the Yale School of Medicine is a...
Click here to add this to my saved trials