Type 1 Diabetes Mellitus Clinical Trial
Official title:
hOKT3γ1 (Ala-Ala), Sirolimus and Low Dose Tacrolimus Therapy in Type 1 Diabetic Islet Allograft Recipients
This clinical trial is designed to extend the observations made in our pilot clinical trial (IND 8971, Study #1) on the safety and efficacy of immunotherapy with the anti-CD3 monoclonal antibody hOKT3γ1 (Ala-Ala), (currently called MGA031) combined with sirolimus and tacrolimus in preventing rejection and autoimmune destruction of deceased donor pancreatic islet transplants in type 1 diabetic recipients.
Type 1 diabetes mellitus continues to be a therapeutic challenge. Previous studies have
shown that failure to prevent hypoglycemia and hyperglycemia results in acute and chronic
complications, leading to poor quality of life, premature death, and considerable health
care costs in 30% to 50% of diabetic patients. Therefore, establishing safe and effective
ways to achieve and maintain normoglycemia would have substantial implications for the
well-being of individuals with diabetes. Intensive insulin therapy has been shown to reduce
the risk of chronic complications in patients who achieve near-normalization of glycemia.
However, such therapy is labor-intensive, difficult to implement for many patients, and
limited by the accompanying increased frequency of severe hypoglycemia. Currently, the only
way to restore and sustain normoglycemia without the associated risk of hypoglycemia is by
replacing the patient's islets of Langerhans, either by transplanting a vascularized
pancreas or, much less invasively, by infusing isolated islets.
Strategies that selectively inactivate autoreactive T cells and prevent allorejection of
transplanted islets in the absence of diabetogenic side effects need to be developed for
islet transplants to survive in autoimmune diabetic recipients. The current clinical study
will extend the observations made in our first pilot clinical trial (IND 8971, Study #1)
that provided preliminary information on the safety and efficacy of immunotherapy with the
anti-CD3 monoclonal antibody hOKT3γ1 (Ala-Ala), (currently called MGA031) combined with
sirolimus and tacrolimus in preventing rejection and autoimmune destruction of deceased
donor pancreatic islet transplants in type 1 diabetic recipients.
In the pilot study 4 of 6 single islet transplant recipients remained insulin independent
with normal HbA1c and no episodes of hypoglycemia throughout the 1 year post-transplant
period. Three of those four participants have maintained insulin independence for > 3.5,
>4.5 and >5 years post islet transplant. These preliminary findings warrant an extension
study involving more recipients and more comprehensive immunologic monitoring to examine in
greater detail the impact of MGA031 induction immunotherapy on T cell responses operative in
rejection and autoimmune destruction of transplanted islets as well as on formation of
regulatory T cell function for the protection of transplanted islets.
A total of 5 patients with type 1 diabetes will be transplanted under this protocol. Islet
transplant recipients will be admitted for 5 days and followed for one year after
transplantation.
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Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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