Evaluate Efficacy Study of Combination Therapy of Everolimus and Low Dose Tacrolimus in Renal Allograft Recipients

Kidney; Complications, Allograft Clinical Trial

— PROTECT  

Official title:

To Evaluate Prevention Effect Of Everolimus and Low-dose Tacrolimus in Comparison With Standard-dose Tacrolimus Therapy With Mycophenolic Acid on the New Onset Diabetes Mellitus After Transplantation in the Renal Allograft Recipients

Clinical Trial Details — Status: Recruiting

Administrative data

• NCT number: NCT02036554
• Other study ID #: CRAD001AKR11T
• Status: Recruiting
• Phase: Phase 4
• First received: December 23, 2013
• Last updated: September 22, 2014
• Start date: March 2013
• Est. completion date: December 2015

Study information

• Verified date: September 2014
• Source: Seoul St. Mary's Hospital
• Contact: n/a
• Is FDA regulated: No
• Health authority: Korea: Food and Drug Administration
• Study type: Interventional

Clinical Trial Summary

To evaluate prevention effect of combination therapy of Everolimus and low-dose Tacrolimus in comparison with standard-dose Tacrolimus therapy with Mycophenolic acid on the New Onset Diabetes Mellitus after transplantation in the renal allograft recipients

Description:

An open-label, randomized, multi-center, comparative parallel study to evaluate prevention effect of combination therapy of Everolimus and low-dose Tacrolimus in comparison with standard-dose Tacrolimus therapy with Mycophenolic acid on the New Onset Diabetes Mellitus after transplantation in the renal allograft recipients: PROTECT study

Recruitment information / eligibility

• Status: Recruiting
• Enrollment: 234
• Est. completion date: December 2015
• Est. primary completion date: December 2015
• Accepts healthy volunteers: No
• Gender: Both
• Age group: 20 Years and older

Eligibility

Inclusion Criteria:

1. Age = 20 year old

2. At least 3 months after kidney transplantation

3. Subject who is using Tacrolimus ± purine synthesis inhibitor + steroid without change within the past 3 months (except the dosage)

4. MDRD eGFR = 50 mL/min or serum creatinine < 2.0mg/dL within the past 3 months in the 6months after kidney transplantation

5. Rate of change of serum creatinine < +30% within the past 3 months in the 6months after kidney transplantation (if serum creatinine decreased, without rate of change is inclusion possible. if serum creatinine result was normal,regardless of the rate of change is able to register.)

6. Urine protein/creatinine ratio < 1g/g Cr (spot urine) Subject who is not applicable to the diagnostic criteria NODAT on

7. the baseline in the 6months after kidney transplantation

8. Subjects who agree with written informed consent

Exclusion Criteria:

1. Subjects who received combined non-renal transplantation

2. Subject who received re-transplantation

3. ABO blood group incompatible(when anti-ABO Antibody titer <1:128 is inclusion possible.)

4. Sensitized patients before transplantation

• Pretransplant or peak PRA titer > 50%

• Pretransplant T cell cytotoxicity crossmatch (+)

5. HLA-identical living related donor

6. Subject who has diabetes mellitus / NODAT before transplantation

7. Subject who has suffered acute rejection episode within the past 3 months in the 6months after kidney transplantation

8. Subject with hypersensitivity to everolimus

9. Subject who should continue nephrotoxic drug until enrollment (Aminoglycoside, amphotericin B, cisplatin)

10. Subject with GI disorder that might interfere with the ability to absorb oral medication. (eg, gastrectomy or insufficiently treated diabetic gastroenteropathy)

11. Subjects with active peptic ulcer

12. HIV, HBsAg, or HCV Ab tests (+)

13. Abnormal liver function test (AST or ALT or total bilirubin> upper normal limit x3)

14. ANC <1.5*109/L or WBC <2.5*109/L or platelet <75*109/L

15. Treatment with an investigational drug within 30 days preceding the first dose of trial medication

16. Women who are either pregnant, lactating, planning to become pregnant in the next 12 months.

17. Subjects with history of cancer(except successfully treated), localized nonmelanocytic skin cancer, PTLD(Post-transplant lymphoproliferative disorder)

18. Subjects with clinically significant infections within the past 4 weeks in the 6months after kidney transplantation

19. Subjects who took major surgery within the past 4 weeks in the 6months after kidney transplantation

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention

Related Conditions & MeSH terms

• Kidney; Complications, Allograft

Intervention

Drug:
• Everolimus
Decrease the level of Tacrolimus and add on Everolimus instead of Mycophenolic acid which is standard treatment.
• Tacrolimus
Decrease the level of Tacrolimus and add on Everolimus instead of Mycophenolic acid which is standard treatment.
• Mycophenolic acid
Decrease the level of Tacrolimus and add on Everolimus instead of Mycophenolic acid which is standard treatment.

Locations

Country	Name	City	State
Korea, Republic of	division of nephrology;Seoul St Mary's Hospital	Seoul

Sponsors (2)

Lead Sponsor	Collaborator
Seoul St. Mary's Hospital	Novartis

Country where clinical trial is conducted

Korea, Republic of, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Primary	Change from Baseline in Development of NODAT (Fasting glucose = 126 mg/dL, Random glucose = 200 mg/dL) at 12 months	To evaluate prevention effect of combination therapy of Everolimus and low-dose Tacrolimus in comparison with standard-dose Tacrolimus therapy with Mycophenolic acid on the New Onset Diabetes Mellitus after transplantation at 12 months after date of randomization.	0 to 12 month	No
Secondary	Insulin resistance by HOMA-IR	Change from Baseline(V2) in Insulin resistance by HOMA-IR at 12months(V6)	0 to 12 months	No
Secondary	Insulin secretion by HOMA-beta	Change from Baseline(V2) in insulin secretion by HOMA-beta at 12 months(V6)	0 to 12 months	No
Secondary	OGTT (Fasting and PP2hr)	Change from baseline in OGTT (Fasting and PP2hr) at 12 months(V6)	0 to 12 months	No
Secondary	Needs for anti-diabetic medication or insulin	Needs for anti-diabetic medication or insulin at Baseline(V2)	at Baseline(V2)	No
Secondary	Needs for anti-diabetic medication or insulin at 3 month(V3)	Needs for anti-diabetic medication or insulin at 3 month(V3)	at 3 month(V3)	No
Secondary	Needs for anti-diabetic medication or insulin at 6 month(V4)	Needs for anti-diabetic medication or insulin at 6 month(V4)	at 6 month(V4)	No
Secondary	Needs for anti-diabetic medication or insulin at 9 month(V5)	Needs for anti-diabetic medication or insulin at 9 month(V5)	at 9 month(V5)	No
Secondary	Needs for anti-diabetic medication or insulin at 12 month(V6)	Needs for anti-diabetic medication or insulin at 12 month(V6)	at 12 month(V6)	No
Secondary	Creatinine clearance (MDRD eGFR) at Baseline(V2)	Creatinine clearance (MDRD eGFR) at Baseline(V2)	at Baseline(V2)	No
Secondary	Creatinine clearance (MDRD eGFR) at 3 month(V3)	Creatinine clearance (MDRD eGFR) at 3 month(V3)	at 3 month(V3)	No
Secondary	Creatinine clearance (MDRD eGFR) at 6 month(V4)	Creatinine clearance (MDRD eGFR) at 6 month(V4)	at 6 month(V4)	No
Secondary	Creatinine clearance (MDRD eGFR) at 9 month(V5)	Creatinine clearance (MDRD eGFR) at 9 month(V5)	at 9 month(V5)	No
Secondary	Creatinine clearance (MDRD eGFR) at 12 month(V6)	Creatinine clearance (MDRD eGFR) at 12 month(V6)	at 12 month(V6)	No
Secondary	12 month graft survival	After date of randomization, evaluate graft survival rate at 12 months(V6)	at 12 months(V6)	No
Secondary	12 month patient survival rate	After date of randomization, evaluate patient survival rate at 12 months(V6)	at 12 months(V6)	No
Secondary	Change from baseline in Microalbuminuria(MAU) at 12 months	Change from baseline in Microalbuminuria(MAU) at 12 months	at 12 months(V6)	No
Secondary	Proportion of patients with significant proteinuria greater than 1g/gCr at Baseline(V2)	Proportion of patients with significant proteinuria greater than 1g/gCr at Baseline(V2)	at Baseline(V2)	No
Secondary	Proportion of patients with significant proteinuria greater than 1g/gCr at 3 month(V3)	Proportion of patients with significant proteinuria greater than 1g/gCr at 3 month(V3)	at 3 month(V3)	No
Secondary	Proportion of patients with significant proteinuria greater than 1g/gCr at 6 month(V4)	Proportion of patients with significant proteinuria greater than 1g/gCr at 6 month(V4)	at 6 month(V4)	No
Secondary	Proportion of patients with significant proteinuria greater than 1g/gCr at 9 month(V5)	Proportion of patients with significant proteinuria greater than 1g/gCr at 9 month(V5)	at 9 month(V5)	No
Secondary	Proportion of patients with significant proteinuria greater than 1g/gCr at 12 month(V6)	Proportion of patients with significant proteinuria greater than 1g/gCr at 12 month(V6)	at 12 month(V6)	No
Secondary	Number of episode of biopsy proven acute rejection (BPAR)	Cumulative incidence rate of Biopsy Proven Acute Rejection(BPAR) at 12months(V6) after date of randomization.	at 12 month(V6)	No
Secondary	Number of hospitalization of any cause (except admission for protocol biopsy) at Baseline(V2)	Number of hospitalization of any cause (except admission for protocol biopsy) at Baseline(V2)	at Baseline(V2)	No
Secondary	Number of hospitalization of any cause (except admission for protocol biopsy) at 3 month(V3)	Number of hospitalization of any cause (except admission for protocol biopsy) at 3 month(V3)	at 3 month(V3)	No
Secondary	Number of hospitalization of any cause (except admission for protocol biopsy) at 6 month(V4)	Number of hospitalization of any cause (except admission for protocol biopsy) at 6 month(V4)	at 6 month(V4)	No
Secondary	Number of hospitalization of any cause (except admission for protocol biopsy) at 9 month(V5)	Number of hospitalization of any cause (except admission for protocol biopsy) at 9 month(V5)	at 9 month(V5)	No
Secondary	Number of hospitalization of any cause (except admission for protocol biopsy) at 12 month(V6)	Number of hospitalization of any cause (except admission for protocol biopsy) at 12 month(V6)	at 12 month(V6)	No
Secondary	Number of opportunistic infections (BKVN) at Baseline(V2)	Number of opportunistic infections (BKVN) at Baseline(V2)	at Baseline(V2)	No
Secondary	Number of opportunistic infections (BKVN) at 12month(V6)	Number of opportunistic infections (BKVN) at 12month(V6)	at 12 month(V6)	No
Secondary	Prevalence of NODAT at Baseline(V2)	Prevalence of NODAT at Baseline(V2)	at Baseline(V2)	No
Secondary	Prevalence of NODAT at 3 month(V3)	Prevalence of NODAT at 3 month(V3)	at 3 month(V3)	No
Secondary	Prevalence of NODAT at 6 month(V4)	Prevalence of NODAT at 6 month(V4)	at 6 month(V4)	No
Secondary	Prevalence of NODAT at 9 month (V5)	Prevalence of NODAT at 9 month (V5)	at 9 month (V5)	No
Secondary	Prevalence of NODAT at 12 month(V6)	Prevalence of NODAT at 12 month(V6)	at 12 month(V6)	No