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Islet Allotransplantation in Type 1 Diabetes

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The Ohio State University

Status and phase

Suspended
Phase 1

Conditions

Type 1 Diabetes

Treatments

Drug: Human Pancreatic Islets

Study type

Interventional

Funder types

Other

Identifiers

NCT01705899
IRB 2006H0200

Details and patient eligibility

About

Islet transplantation can provide physiologic insulin replacement to patients with type 1 diabetes without the complications associated with whole pancreas transplantation. The purpose of this study is to achieve insulin-independence in patients with type 1 diabetes, thereby eliminating the need for exogenous insulin injections to maintain normal glucose levels, ameliorating severe hypoglycemia and potentially decreasing the development of diabetes-related complications. This study will investigate islet transplantation in subjects who have preserved renal function and subjects who have undergone cadaveric renal transplantation, since the latter subjects are already on immunosuppression.

This is a single center, prospective trial of islet transplantation in subjects receiving islets alone or islets after kidney transplant. This is a phase I study investigating the use of islet transplantation for the treatment of type 1 diabetes. Subjects will be eligible for an islet transplant if they meet all of the inclusion criteria and none of the exclusion criteria outlined in the protocol. In brief, the aims of this study are to establish an islet transplant program at the Ohio State University, determine the safety of islet transplantation in islet alone and kidney transplant recipients, determine whether islet transplantation will reduce the frequency of severe hypoglycemic events, determine whether a novel steroid-free immunosuppressive protocol will prevent rejection in islet transplants and to achieve insulin independence at one year after the final islet transplant.

Full description

Hypothesis - Insulin independence (insulin injections no longer needed) will be achieved in subjects with type 1 diabetes receiving islet transplantation using the immunosuppressive regimen of cyclosporine and sirolimus. Amelioration of severe hypoglycemia will also be achieved in these groups.

Primary Objective

To determine the safety of islet transplantation in islet alone and in kidney transplant recipients. Safety analyses include:

  • Incidence, timing and severity of adverse events and their relationship to the transplant protocol, islet infusion and immunosuppressive medications
  • Proportion without protocol-related serious adverse events (SAE) at 1 year
  • Incidence, type and severity of infectious complications
  • Incidence and severity of procedural-related events, such as bleeding and portal vein thrombosis
  • Incidence and severity of liver function test elevations
  • Incidence and severity of hypoglycemia
  • Incidence and severity of creatinine clearance and urine microalbumin changes
  • Incidence and severity of lipid abnormalities
  • Proportion of those who develop donor-specific alloantibody

Secondary Objective

To determine the efficacy of islet transplantation in islet alone and in kidney transplant recipients. Efficacy analyses include:

  • Time to insulin independence, defined as freedom from insulin use (insulin injections not needed) for 14 or more consecutive days

  • Proportion of those that achieve insulin independence at any time during the first year

  • Proportion of those one year after final transplant who have:

    • Positive C-peptide (≥0.3 ng/ml after stimulation)
    • Full function of their graft
    • Partial function of their graft
    • Marginal function of their graft
    • Mixed meal stimulated C-peptide >1.0 ng/ml at 6, and 12 months

  • Proportion of those that have an acute insulin response to glucose (AIRg) >20uU/ml during frequently sampled intravenous glucose tolerance test (FSIGT) at 6 and 12 months

  • Proportion of those with blood glucose level <140 mg/dl two hours after oral glucose tolerance test (OGTT) at 6 and 12 months

  • Proportion of those that have improved QOL at 6 and 12 months compared with baseline

  • Proportion of those that have improved hypoglycemia and glycemic lability scores at 6 and 12 months compared with baseline

Definition of full islet function:

  • Insulin independence
  • A1C ≤ 6.5%
  • Absence of severe hypoglycemic episodes
  • Fasting glucose ≥140 mg/dl less than 3 times a week
  • Post-prandial glucose (2 hours) >180 mg/dl less than 4 times a week

Definition of partial islet function:

  • Insulin requirement less than 50% of pre-transplant insulin requirement
  • C-peptide positive (≥0.3 ng/ml after stimulation)
  • A1C ≤ 6.5%
  • No severe hypoglycemia

Definition of marginal islet function:

  • C-peptide positive (≥0.3 ng/ml after stimulation)
  • A1C ≤ 7.5%
  • No severe hypoglycemia

This trial will have two study groups consisting of N=10 subjects with type 1 diabetes. One group (IA) will include subjects with preserved kidney function. A second group (IAK) will include subjects with renal failure secondary to diabetes who have received a prior kidney transplant at least 6 months previously and have stable renal function on a steroid-free immunosuppressive regimen.

Potential study participants will be recruited from the Endocrinology and Transplant clinics at the Ohio State University, and community physician referrals. Those who are potentially eligible will undergo a screening evaluation after review of the medical records. If the subject remains eligible, he/she will be enrolled in the islet transplant study and will be placed on a waiting list for an islet transplant. Once a transplant becomes available, the subject will be admitted to the hospital to undergo the transplant procedure. Frequent follow-up visits in the transplant clinic will occur throughout the following year after the transplant. Subjects will be closely monitored for adverse events and insulin requirements. If the subject does not achieve insulin independence, he/she may be eligible for a subsequent transplant.

There will be a 10-year enrollment with 12-month follow-up after last transplant. Since subjects may be eligible for a subsequent transplant within 18 months of the first transplant, the total duration may be up to 30 months after the first transplant in some subjects.

The study will be completed one year after the last islet transplant. Subjects who have undergone the islet transplant procedure and have completed the post-transplant evaluations one year after their last transplant will be considered to have completed the study.

Read more

Enrollment

20 estimated patients

Sex

All

Ages

18 to 65 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

  1. Type 1 diabetes > 5 years

  2. First islet transplant

  3. Demonstrate intensive efforts to manage diabetes for last 6 months (≥4 SMBG/day, ≥3 injections of insulin/day or use of pump and ≥3 contacts with diabetes care team in last 12 months)

  4. Metabolic complications: at least one of the following:

    •Reduced hypoglycemia awareness (inability to sense hypoglycemia until blood glucose falls to < 54 mg/dl or > one hypoglycemic episode in last 12 months requiring outside help and not explained by clear precipitant)

    •≥2 severe hypoglycemic events or ≥2 hospitalizations for diabetic ketoacidosis (DKA) in last year.

  5. Ability to provide written informed consent

  6. Age 18-65

  7. Specific for group 2: All of above (1-6) with renal transplant at least 6 months previous

Exclusion criteria

  1. Age < 18 years or > 65 years
  2. Inability to provide informed consent
  3. Body Mass Index > 29 kg/m2
  4. Insulin requirement of > 50 units/day
  5. Stimulated C-peptide ≥ 0.2 ng/ml
  6. Current panel reactive anti-HLA antibodies >20%
  7. Cardiovascular instability
  8. Previous islet transplant
  9. History of malignancy except squamous and basal cell skin cancer unless disease-free for > 2 years determined by independent oncologist
  10. Active peptic ulcer disease
  11. Condition that may interfere with absorption of medications
  12. Hemoglobin A1C > 12%
  13. Invasive aspergillus infection within one year
  14. Varicella titer index <1.0
  15. Rubella titer <10 IU/ml
  16. Psychiatric disorder
  17. Untreated hyperlipidemia: fasting total cholesterol >240 mg/dl, low density lipoprotein>130 mg/dl, or triglycerides >200 mg/dl
  18. Hemoglobin <10 g/dl for females, and <11 g/dl for males, white blood cell count < 3,000/µL, platelet count of <150,000/microliter, CD4+ count <500/microliter
  19. Liver function test abnormalities (if any value > 1.5 times normal, candidate will be excluded. If 1-1.5 times normal, test will be repeated. If re-test value remains above normal, candidate will be excluded).
  20. Prostate specific antigen >4.0 ng/ml
  21. Presence of gallstones, liver hemangioma, cirrhosis or evidence of portal hypertension
  22. Untreated proliferative diabetic retinopathy
  23. Females: positive pregnancy test, intent for future pregnancy, or any subject of reproductive age who is not surgically sterile and is unable or unwilling to use acceptable method of contraception
  24. Female subjects who are breast-feeding
  25. Adrenal insufficiency: 8am cortisol >19 mcg/dl adequate. Values 19 mcg/dl will be followed by Adreno-Corticotropic Hormone stimulation test
  26. Any disease or condition that requires use of chronic steroids
  27. Coagulopathy or use of chronic anticoagulation
  28. Hyperthyroidism unless treated with radioactive iodine or surgery
  29. Thyroid function tests outside normal range
  30. Active alcoholism or other substance abuse within the past six months
  31. History of non-adherence. Questionable adherence requires agreement entered and compliance demonstrated for at least 3 months
  32. Active infection including hepatitis B or C, human immunodeficiency virus positive, positive Mantoux test [unless previously immunized with Bacillus Calmette-Guerin], or X-ray evidence of pulmonary infection
  33. Inability to reach hospital within 6 hours of notification
  34. Failure to clear psychological or psychiatric screen
  35. Medical condition or circumstance that investigator finds will interfere with safe completion of the study

Exclusion criteria specific for group 1:

  1. Receipt of previous transplant (excluding pancreas)
  2. Creatinine clearance <50 ml/minute for females and <60 ml/minute for males or macroalbuminuria (>500 mg/24h)

Exclusion criteria specific for group 2:

  1. Creatinine clearance <40ml/minute
  2. Renal transplant in last 6 months
  3. Current use of corticosteroids

Trial design

Primary purpose

Treatment

Allocation

Non-Randomized

Interventional model

Parallel Assignment

Masking

None (Open label)

20 participants in 2 patient groups

Subjects with preserved kidney function
Experimental group
Description:
Subjects with preserved renal function that have not previously received a kidney transplant will be treated with Human Pancreatic Islets (in the form of islets alone - IA).
Treatment:
Drug: Human Pancreatic Islets
Subjects with prior kidney transplant
Experimental group
Description:
Subjects with renal failure secondary to diabetes who have received a prior kidney transplant at least 6 months previously and have stable renal function on a steroid-free immunosuppressive regimen will receive Human Pancreatic Islets (in the form of islets after kidney - IAK).
Treatment:
Drug: Human Pancreatic Islets

Trial contacts and locations

1

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Data sourced from clinicaltrials.gov

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