Hyperglycemia Clinical Trial
Official title:
Insulin Therapy for the Prevention of New Onset Diabetes After Transplantation (ITP-NODAT) Prospective Study in Non-Diabetic De Novo Kidney Transplant Recipients
This study aims to assess the effects of early basal insulin therapy in previously non-diabetic de novo kidney transplant patients in reducing the incidence of new onset diabetes in particular and abnormal glucose metabolism in general during subsequent follow-up.The ITP NODAT study should be seen in connection with the Vienna SAPT-NODAT study (clinicaltrials.gov record number: NCT01680185), as for the final analysis, the data yielded from the three arms in those two studies will be used for an pooled analysis.
New-onset diabetes after transplantation (NODAT) is strongly associated with postoperative
hyperglycemia, and reduced patient as well as graft survival. In our recent proof-of-concept
clinical trial (TIP), we have shown that immediate post-transplant basal insulin therapy
decreases hyperglycemia and reduces the prevalence of NODAT by improving pancreatic β-cell
function.
In consequence, this study as an interventional trial comparing aggressive glycemic control
with early institution of insulin therapy to standard of care (dietary precaution, life-style
modification, oral hypoglycemic agents and/or insulin as needed) aims to assess the effects
of early basal insulin therapy in previously non-diabetic de novo kidney transplant patients
in reducing the incidence of new onset diabetes in particular and abnormal glucose metabolism
in general during subsequent follow-up.
Patients will be enrolled through the University of Michigan and the Medical University of
Vienna, Austria (MUV), who is the official sponsor of the European part of the ITP-NODAT
study. This record only refers to the European part of the ITP-NODAT study, specifically to
all study patients from the following study Centers: MUV; Medical University of Graz,
Austria; Charité Berlin, Germany; Hospital Del Mar, Barcelona, Spain. For the patients
enrolled through the University of Michigan (i.e., the US-part of the ITP-NODAT study), a
separate records exists (responsible PI: Dr. Akinlolu Ojo).
This study will involve previously non-diabetic ESRD patients undergoing kidney
transplantation with either a deceased or living donor kidney who will receive standard
triple immunosuppression regimen including a calcineurin inhibitor (once-daily tacrolimus in
Europe, twice-daily tacrolimus in the U.S.), an anti-metabolite (mycophenolate mofetil) and
corticosteroids (prednisone) and be followed at each transplant center's outpatient clinic
for at least 2 years following transplantation according to the established standard center
protocol.
Methods: Combining the study presented here (ITP-NODAT) and the SAPT-NODAT study mentioned
above will yield three study arms, with 28 patients in each arm, namely: [1] the control arm,
treated by standard-of-care; [2] the basal insulin arm, treated predominantly with
intermediate acting NPH insulin (human insulin isophane, Humulin N, Eli Lilly); [3] the SAPT
arm, treated with short acting insulin (Insulin lispro, Humalog, Eli Lilly), applied
continuously by SAPT technology. Adult patients with absence of diabetes will be randomized
prior to renal transplantation and stratified by deceased donor or living donor, if they are
capable of understanding the study and are willing to give informed written consent for all
three study arms. Patients will receive standard triple immunosuppressive medications
(twice-daily tacrolimus, mycophenolate mofetil or mycophenolic sodium and steroids) with
predefined tacrolimus targets and steroid doses. The algorithm for insulin administration is
designed to account for the prominent evening peak of hyperglycemia observed in our previous
TIP-study. The primary endpoint is HbA1c (in rel.%), at 3 months, and superiority will be
assumed if a statistically significant difference between the SAPT-treatment group versus the
standard-of-care control group can be determined, by two-sided Student's t-test. Secondary
endpoints will be compared between all three groups and will include hypoglycemic events,
glycemic variability, 2h glucose ≥200 mg/dL (by oral glucose tolerance test [OGTT] to
determine prevalence of diabetes, prediabetes and normal glucose tolerance), beta cell
function and insulin sensitivity derived from OGTT, serum creatinine, quality of life
measures, patient and graft survival. All secondary endpoint comparisons relying on OGTTs
will be made at 6, 12 and 24 months after kidney transplantation, respectively. The result of
the 6-months OGTT will be blinded to patients and investigators to prevent subsequent
treatment bias.
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