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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT01094613
Other study ID # Protocol C2/13/DR-6MP-02
Secondary ID
Status Terminated
Phase Phase 1/Phase 2
First received March 25, 2010
Last updated March 6, 2013
Start date November 2010
Est. completion date December 2012

Study information

Verified date March 2013
Source Teva GTC
Contact n/a
Is FDA regulated No
Health authority Israel: Ethics CommissionIsrael: Ministry of Health
Study type Interventional

Clinical Trial Summary

The study is designed to evaluate the clinical efficacy and safety of daily treatment for 12 weeks of oral administration of a delayed release, locally delivered 6MP (mercaptopurine) drug (80 mg), as compared to standard Purinethol (at a dose of 1-1.5 mg/kg/body weight), in alleviating the clinical, immunological and mucosal signs and symptoms of moderately active Crohn's Disease


Description:

Crohn's Disease (CD) therapy is aimed at reducing inflammation via induction of remission after a flare-up and maintenance of the remission for as long as possible. Therapies commonly used for inducing remission are steroids and anti-TNF-a. Standard 6MP, on the other hand, has a slow onset of action and requires several months of administration before its therapeutic effects become apparent. Therefore, 6MP is typically used as maintenance therapy, rather than for remission. Furthermore, serious AE's associated wtih 6MP include leucopenia, hepatoxicity, pancreatitis and bone marrow suppression, requiring lowering of dose or treatment discontinuation.

The Teva DR-6MP project was designed to evaluate a new oral 6MP formulation that would address these limitations. The slow action of standard 6MP, precluding its use as a treatment for induction of remission, would be offset by a faster-disintegrating, more soluble formulation with an enteric coating for targeted ileal delivery. This new formulation designed to open at the terminal ileum, the most commonly affected area of CD bowel involvement, could deliver higher effective local concentrations of drug to the site most affected by CD, stimulating an effective local immunological response, resulting in a cascade of widespread immunological activity, evoking an induction of remission. The safety of standard 6MP would be improved upon by the fact that negligible levels of the DR-6MP formulation have been observed in the plasma, obviating the toxicities associated with systemic 6MP. Moreover, since the DR-6MP dose is fixed and not subject to patient weight, nor potentially, side-effects, the dose adjustments required for up-titration to optimal dose, or down-titration due to toxicity, could be avoided.

Previous small, pilot proof-of-concept clinical efficacy and pharmacokinetic studies of the DR-6MP formulation demonstrated the potential for induction of remission, mucosal healing, systemic immunological improvement and lower systemic side-effects.

The current study is designed to repeat the earlier studies under larger, more rigorous conditions in a randomized, double-blind fashion at multiple sites to ascertain if the initial encouraging results could be repeated. Moreover, a higher dose of 6MP (80 mg) will be tested to ascertain if presumably higher local concentrations at the disease site can evince a more robust clinical effect.


Recruitment information / eligibility

Status Terminated
Enrollment 70
Est. completion date December 2012
Est. primary completion date December 2012
Accepts healthy volunteers No
Gender Both
Age group 18 Years to 75 Years
Eligibility Inclusion Criteria:

1. Male or (non-pregnant) female, 18-75 years (incl) at screen.

2. Diagnosed w/CD, appropriately documented/supported by endoscopy or radiology.

3. W/ moderately active CD, w/ screen CDAI score 220-450 (inclusive)

4. Screen lab tests:

- HGB >/= 8.5 g/dL,

- Platelets >/= 100,000/ mm³

- WBC >/= 3500 mm³

- Serum albumin > 2.5 g/dL

- ALT, AST, ALK Phos, GGTP,. total and direct bilirubin < 2xULN

5. Subjects may be on stable (for at least 2 wks prior screen) 5-ASA, chronic antibiotics or low-dose oral steroids (prednisolone-up to 15 mg daily; budesonide-up to 6 mg daily) and remain on the drug at that dose throughout the study

6. Willing and able to provide written ICF.

Exclusion Criteria:

1. W/ ulcerative colitis or w/ diagnosis of indeterminate colitis.

2. W/ previous bowel resection due to CD resulting in clinically significant Short Bowel Syndrome.

3. W/ fistulizing CD w/ clinic or radiologic evidence of abscess.

4. W/ clinically significant GI obstructive symptoms or x-ray evidence of fibrosed bowel.

5. W/ screen stool culture + for enteric pathogens (Salmonella, Shigella, Campylobacter) or Clostridium difficile toxin assay.

6. W/ hx of persistent intestinal obstruction, bowel perforation, uncontrolled GI bleed,abdominal abscess,infection or toxic megacolon.

7. W/ hx of GI tract malignancy or IBD-associated malignant intestinal changes.

8. W/ surgery/major procedure in 4 weeks prior to 1st study dose.

9. Receiving elemental diet or parenteral nutrition.

10. W/ current signs/symptoms of clinically significant/unstable med/surg condition that precludes safe/complete study participation, determined by med history, PE, ECG, lab tests or imaging. Such conditions may include severe, progressive or uncontrolled renal, metabolic, hepatic, hematologic, endocrine, pulmonary, cardiovascular, psychiatric, neurologic, cerebral or autoimmune disease.

11. W/ serious infections, such as hepatitis, pneumonia, pyelonephritis w/in 12 weeks prior to 1st study dose. Less serious infections such as acute UR tract infections or uncomplicated UT infection not considered exclusions - at discretion of PI.

12. W/ currently known malignancy/pre-malignant lesions/hx of malignancy w/in past 5 years, excl basal cell carcinoma.

13. W/ hx of coagulopathy.

14. W/ porphyria as it may interfere w/ assessment of CD abdominal pain.

15. W/ hx of previous thiopurine failure resulting in serious AE (ex: severe pancreatitis, leucopenia, hepatoxicity or bone marrow suppression) so as to preclude addtl tx w/ 6MP at any dose

16. Taking w/in 6 months prior to 1st study dose (+during study) Active vaccinations (live attenuated bacterial/viral pathogens)

17. Taking w/in 6 weeks prior to 1st study dose (+ during study):

- Anti-TNFa (infliximab, etanercept, adalimumab)

- Anti-integrin (natalizumab)

- Anti-neoplastics, incl methotrexate, daunorubicin hydrochloride

18. Taking w/in 4 weeks prior to 1st study dose (+ during study):

- Immunosuppressants such as AZA, 6-MP (i.e., other than 6MP drug assigned during study), cyclosporine, tacrolimus, mycophenolate mofetil or thalidomide.

- Antibiotics or oral/IV corticosteroids (other than oral prednisolone allowed during study as rescue therapy as per protocol).

- Tx w/ drugs known to induce/inhibit endogenous hepatic drug metabolism such as barbiturates, phenothiazines, cimetidine, carbamazepine etc.

- Anti-coagulant therapy such as: heparin, warfarin, acenocoumarol.

- Medications that induce blood dyscrasias or w/ potential for immune dysfunction, bone marrow depression and/or symptoms of CD (diarrhea, abdominal pain).

- Vaccinations involving inactivated forms of pathogens or purified antigenic proteins (Note: passive immunization involving antibody inoculations permitted at any time)

19. Tx w/in 2 wks prior to 1st study dose (+ during study) IV or oral steroids (prednisolone or budesonide) Antibiotics

Note: 2 impt exceptions (a) Subjects oral steroid or antibiotic dependent with active CD (CDAI 220-450)in spite of these txs, may remain on tx provided on stable (>=2wks at screen)dose and remain at that dose throughout study (b) Subjects who require steroid-rescue during study

20. Taking w/in 7 days prior to 1st study dose (+ during study):

- Anticholinergic or other drugs known to affect GI motility.

- Allopurinol

- Proton pump inhibitors or other drugs affecting gastric acidity

21. W/body weight below 42.5 kg.

22. Pregnant/nursing at screen, or intend to be during study.

23. Women of childbearing potential not practicing acceptable method of birth control [acceptable methods: surgical sterilization, IUD, contraceptive (oral, patch, or long-acting injectable), partner's vasectomy, double-protection method (condom or diaphragm w/ spermicide) or abstinence].

24. W/ current/hx of drug and/or alcohol abuse.

25. Largely or wholly bed-ridden and w/ little capacity for self-care.

26. W/ known allergy or hypersensitivity to 6-MP or any inactive component of study drug (ex: lactose intolerant).

27. Participated in other clinical trial using investigational drugs w/in 12 weeks prior to 1st study dose.

28. W/ planned elective surgery or hospitalization during study (that may interfere w/ study compliance/outcome).

29. W/inability to communicate well w/investigators/staff (i.e., language problem, poor mental development or impaired cerebral function).

30. Unavailable for trial duration, unable to comply w/schedule, likely to be noncompliant, or felt unsuitable by PI for any other reason.

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator, Outcomes Assessor), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
Delayed Release 6 mercaptopurine
Delayed Release oral tablet for ileal drug delivery, 80 mg, once nightly before bedtime, for 12 weeks. Since the study drug must be blinded, patients randomized to this arm will receive the following: 80 mg DR-6MP: 2 active 40 mg DR-6MP tablets.
6 Mercaptopurine
Oral tablet(s) to be administered once daily in the AM, for 12 weeks.Purinethol is available only as a 50 mg tablet; patients randomized to this arm will receive varying doses (dependent on baseline body weight and AE profile) throughout the study;and study drug to be blinded. Therefore, patients randomized to this arm to receive combination active Purinethol/comparable placebo. For ex: 50 mg Purinethol= 1 active 50 mg tablet, 2 comparable placebo tablets; 100 mg Purinethol = 2 active 50 mg tablets, 1 placebo tablet; 150 mg Purinethol = 3 active 50 mg tablets. Patients receiving 75 mg or 125 mg will receive alternating daily doses of 50 and 100 mg, or 100 and 150 mg, respectively, to arrive at a weekly average dose of 75 mg or 125 mg.

Locations

Country Name City State
Israel Ha'emek Medical Center Afula
Israel Bnai Zion Hospital Haifa
Israel Rambam Medical Center Haifa
Israel Hadassah Medical Center Jerusalem
Israel Shaarei Tzedek Medical Center Jerusalem
Israel Meir Medical Center Kfar Saba
Israel Holy Family Hospital Nazareth
Israel Kaplan Medical Center Rehovot
Israel Tel Aviv Sourasky Medical Center Tel Aviv
Israel Sheba Medical Center Tel Hashomer
Israel Assaf Harofeh Zerifin

Sponsors (1)

Lead Sponsor Collaborator
Teva GTC

Country where clinical trial is conducted

Israel, 

Outcome

Type Measure Description Time frame Safety issue
Primary Proportion of subjects with clinical response at study end Clinical response is defined as a reduction in CDAI score (Crohn's Disease Activity Index) by 100 points from baseline, or remission (CDAI score <150),even if it is achieved with reduction of CDAI score of less than 100 points from baseline 12 weeks No
Secondary Time to clinical response Although the primary outcome is to assess the proportion of patients with clinical response at Week 12, we are also interested to see how early during treatment (i.e., between weeks 2 and 12), was this clinical response actually achieved for each treatment group, and if it was maintained until the end of the study (week 12) Week 2, 4, 6, 8 or 12 No
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