Bucillamine Phase 2 Trial in Patients With Cystinuria



Status:Recruiting
Conditions:Nephrology
Therapuetic Areas:Nephrology / Urology
Healthy:No
Age Range:18 - 80
Updated:4/15/2017
Start Date:May 2017
End Date:March 2018
Contact:Fabio Chianelli
Email:fabio@revivethera.com
Phone:905-605-5535

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Phase 2 Multi-Center, Dose Escalation Trial To Assess The Safety And Effectiveness Of Bucillamine On Urinary Cystine Excretion And Cystine Capacity In Patients With Cystinuria

Subjects on a standard regimen of tiopronin (cystine binding thiol drug; CBTD) plus
prescribed first-line therapy (i.e. on a hydration, alkali therapy and dietary restriction)
who are failing therapy will be selected for this trial.

After completing informed consent, the subject will have Screening consisting of medication
history and physical examination with vital signs. Samples of blood and urine will be taken
for clinical laboratory and urinalysis. Patients will undergo a 12-lead ECG test. A history
of side effects with current CBTD as well as laboratory recordings of abnormalities
attributable to treatment will also be recorded.

Subjects will be dosed in a sequential manner, starting with the low dose group (300
mg/day), then proceeding to the 600 mg.day dose group.. Safety and tolerability will be
monitored closely by an Independent Medical Monitor (IMM) and based on the IMM's assessment
that it is safe to proceed to the higher dose (600 mg/day), subsequent subjects will be
enrolled into that group. Up to 15 subjects each will be enrolled into either Group A or
Group B.

After 7 days on the assigned bucillamine dose, a 24-hour urine sample will be taken and
after completing the Day 8 safety visit, subjects will undergo a 7 day washout where no
CBTDs will be taken. Thereafter, subjects will be allowed to resume their originally
prescribed CBTDs under Investigator's supervision.

One week following study drug discontinuation, subjects will return to the clinic for
follow-up safety assessments.

Subjects on a standard regimen of tiopronin (cystine binding thiol drug; CBTD) plus
prescribed first-line therapy (i.e. on a hydration, alkali therapy and dietary restriction)
who are failing therapy will be selected for this trial.

Subjects will be encouraged to continue their usual self-selected ad-lib diets, fluid and
alkali regimen and keep this regimen consistent throughout the duration of the study. Study
diaries will be kept to assess consistency and drug compliance.

After completing informed consent, the enrolled subject will have an initial Screening
interview. During the interview the patient will be assessed for symptoms of renal colic as
well as asked about any scheduled urological procedures (a positive indication is an
exclusionary criteria). At the Screening visit, a medication history will be taken and a
complete physical examination, including vital signs will be done. Samples of blood and
urine will be taken for clinical laboratory and urinalysis. Patients will then undergo a
12-lead ECG test.

A history of side effects with current CBTD as well as laboratory recordings of
abnormalities attributable to treatment will also be recorded.

Enrolled subjects will be dosed in a sequential manner, starting with the low dose group
(300 mg/day). Safety and tolerability will be monitored closely by an Independent Medical
Monitor (IMM) and based on the IMM's assessment that it is safe to proceed to the higher
dose (600 mg/day), subsequent subjects will be enrolled into that group. Up to 15 subjects
each will be enrolled into either Group A or Group B.

Subjects will stop taking their current CBTDs for 7 days and perform a 24-hour urine
collection on Day-7 and report for Day 1 Visit .

Subjects enrolled into Group A will start taking bucillamine tablets orally, three times a
day preferably 1hr before or 2hrs after meals in the following sequence; 100 mg (1 tab) in
the morning; 100 mg (1 tab) at noon and 100 mg (1 tab) at night. This drug regimen will
continue for 7 days. Safety Visits are scheduled on Day 3 and Day 8 (End of Study Visit).
Furthermore, on Day 7 a 24-hour urine collection will be performed. Instructions for
handling this sample will be provided in a separate manual.

Subjects enrolled into Group B, will start taking bucillamine tablets orally, three times a
day preferably 1hr before or 2hrs after meals in the following sequence; 200 mg (2 tabs) in
the morning; 200 mg (2 tabs) at noon and 200 mg (2 tabs) at night. This drug regimen will
continue for 7 days. Safety Visits are scheduled on Day 3 and Day 8 (End of Study Visit).
Furthermore, on Day 7 a 24-hour urine collection will be performed. Instructions for
handling this sample will be provided in a separate manual.

After 7 days on the assigned bucillamine dose and after providing the 24-hour urine sample,
and after completing the Day 8 safety visit, subjects will undergo a 7 day washout where no
CBTDs will be taken. Thereafter, subjects will be allowed to resume their originally
prescribed CBTDs under Investigator's supervision.

One week following study drug discontinuation, subjects will return to the clinic for
follow-up safety assessments.

Inclusion Criteria:

1. Subjects of any gender and of any race ≥18 and ≤80 years of age

2. Subjects with proven cystinuria who are failing their standard drug therapy of
tiopronin plus first-line therapy (hydration, alkali and diet restriction) and who
meet the following criteria.

- formed new stones while taking a thiol.

- had increase in stone size of pre-existing stones while taking a thiol.

- had a urologic intervention for stones while taking a thiol

3. Subjects must be able to reliably urinate in a collection vessel and measure urine
volume

4. Subjects must have documentation of a stable complete blood count (CBC) and
urinalysis (UA) in the 6 months prior to date of enrollment

5. Subjects may have a history of but not currently active CNS disorders or
symptoms/effects (e.g., headache)

6. Subjects must have adequate organ function, evidenced by the following laboratory
results within 30 days prior to enrollment:

- Absolute neutrophil count >2000 cells/mm

- Platelet count >140,000 cells/mm3

- Hemoglobin >11.0 g/dl

- Albumin ≥2.5 g/dl

- Total bilirubin ≤1.5 upper limit of normal (ULN)

- SGOT (aspartate aminotransferase [AST]), SGPT (alanine aminotransferase [ALT]),
and alkaline phosphatase (ALP)

≤ 2.5 x ULN

- eGFR >60 ml/min/173m 2 based on Modification of Diet and Renal Disease (MDRD)
Study equation which includes the variables of creatinine, age, sex and race

7. Female subject who has been post-menopausal for at least 24 consecutive months, or
women who have undergone surgical sterilization, (e.g. hysterectomy, bilateral
oophorectomy, tubal ligation or salpingectomy) is eligible without requiring the use
of a contraceptive methods described in Inclusion #8

8. For women of childbearing potential and men with partners of childbearing potential,
agreement to use a highly effective, non-hormonal form of contraception:

- Acceptable forms of should include two of the following:

- Placement of intrauterine device (IUD) or intrauterine system (IUS)

- Condom with spermicidal foam/gel/film/cream/suppository

- Diaphragm or cervical/vault caps with spermicidal
foam/gel/film/cream/suppository

- The above contraception is not a requirement in the case of any of the
following:

- Subject is surgically sterilized

- Subject has had no menstrual period for 12 consecutive months

- Contraception use should continue for the duration of the study treatment and
for at least 3 months after the last dose of study treatment Periodic abstinence
(e.g., calendar ovulation, symptom-thermal, post-ovulation methods) and
withdrawal are not acceptable methods of contraception

9. Subjects must be willing and able to give written informed consent

Exclusion Criteria:

1. Subjects with renal colic

2. Subjects who are scheduled to undergo a surgical procedure

3. Subjects on D-penicillamine (see page 35 for explanation)

4. Subjects with cancer

5. Subjects with acute or chronic infections including HIV, tuberculosis, hepatitis B or
hepatitis C

6. Patients with proteinuria ≥30 mg that is confirmed on repeat laboratory assessment
within 24 hours

7. Subjects with QTc interval >450 ms

8. A history of, hypokalemia and family history of Long QT syndrome

9. Use of concomitant medications that may prolong QT/QTc interval

10. Patients with significant heart failure and activity impairment (Class III-IV of the
New York Heart Association (NYHA)

11. Subjects with serious hepatic disorder (Child-Pugh scores B or C)

12. Subjects with a history of alcohol or substance abuse within the 12 months prior to
enrollment

13. Subjects with history of or active blood dyscrasia such as myelosuppression,
leukopenia, granulocytopenia, thrombocytopenia, pancytopenia, and aplastic anemia.

14. Subjects with Coagulopathy (regardless if controlled by pharmacotherapy or not)

15. Subjects who have any concomitant illness (including active significant infection) or
other finding that, in the opinion of the Investigator, would confound the study data
or place the subject at unacceptable risk if the subject were to participate in the
study, or that would require frequent adjustments in concomitant medications during
the course of the study

16. Use of any investigational drug within 30 days prior to enrollment

17. Subjects currently participating in another research study or anticipated to enroll
in such during participation in this study

18. Subjects for whom informed consent cannot be obtained
We found this trial at
5
sites
1720 2nd Avenue South
Birmingham, Alabama 35294
Principal Investigator: Dean Assimos, MD
Phone: 205-996-2613
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400 Bald Hill Road
Warwick, Rhode Island 02886
401-739-9350
Principal Investigator: Gyan Pareek, MD
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Boston, Massachusetts 02114
Phone: 617-726-7872
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750 Highland Avenue
Madison, Wisconsin 53705
Phone: 360-252-2500
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550 1st Ave
New York, New York 10016
(212) 263-7300
Principal Investigator: Lama Nazzal, MD
Phone: 212-686-7500
New York University School of Medicine NYU School of Medicine has a proud history that...
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