Kidney Transplant Clinical Trial
Official title:
A Prospective, Longitudinal Study to Assess the Metabolic and Renal Effects of Rosiglitazone in Albuminuric Kidney Transplant Recipients
Abnormalities in glucidic and lipidic metabolism are common features in renal transplant patients on chronic immunossupression with steroids and calcineurin inhibitors. In kidney transplant patients with chronic rejection these abnormalities cluster with renal and cardiovascular risk factors and altogether may sustain premature graft loss and may increase the risk of cardiovascular morbidity and mortality. Thiozolidinediones are a new class of oral antidiabetic agents that may increase insulin sensitivity improving the glucose tolerance and dyslipidemia. Moreover, rosiglitazone –one of these drugs- has been reported to decrease blood pressure and albuminuria in subjects with type 2 diabetes and nephropathy. Recent finding that glitazones ameliorate the glucidic and lipidic profile induced by steroid treatment in healthy subjects, provided a further rationale to evaluate the metabolic and renal effects of glitazones in renal transplant patients on chronic steroid therapy. Thus, we designed and organized a pilot study to assess the short-term risk/benefit profile of rosiglitazone in renal transplant patients with chronic rejection. Ten patients will have a basal evaluation of insulin sensitivity, glucose tolerance,lipid profile, renal hemodynamic and albuminuria. These evaluations will be repeated at the end of the treatment (4 months of therapy with rosiglitazone 8 mg/day) period and 2 months after treatment withdrawal.
INTRODUCTION Decreased insulin sensitivity, impaired glucose tolerance and dyslipidemia are
common features in renal transplant patients on chronic immunosuppression with steroids and
calcineurine inhibitors. In renal transplant patients with chronic allograft dysfunction
these metabolic abnormalities typically cluster with well-established renal and
cardiovascular risk-factors such as hypertension and albuminuria. Altogether these factors
may sustain and accelerate the progression of chronic allograft dysfunction to end stage
renal disease (ESRD) and increase the risk of premature cardiovascular morbidity and
mortality.
Thiazolidinediones (glitazones) are a new class of oral antidiabetic agents that may
increase insulin sensitivity through activation of the peroxisome prolipherator-activated
receptor gamma (PPARgamma). By ameliorating insulin sensitivity, these drugs may also
improve glucose tolerance and dyslipidemia. These properties have led to their current
utility as antidiabetic drugs. Moreover, finding that one of these drugs – rosiglitazone –
has been reported to decrease arterial blood pressure and albuminuria in patients with type
2 diabetes and nephropathy, has been taken to suggest that glitazones may also have a
specific reno- and cardio-protective effect. This effect could specifically apply to renal
transplant patients with chronic allograft dysfunction in whom glitazones, in addition to
ameliorate insulin resistance, glucose tolerance and dyslipidemia, might help controlling
arterial hypertension and reducing albuminuria.
Recent finding that glitazones ameliorate the insulin resistant status induced by steroid
treatment in healthy subjects, provides a further rationale to evaluate the metabolic and
renal effects of glitazones in renal transplant patients on chronic steroid therapy.
AIM To evaluate the short-term risk/benefit profile of rosiglitazone treatment in renal
transplant patients with chronic allograft dysfunction.
DESIGN After a basal evaluation of systolic/diastolic blood pressure,body weight, insulin
sensitivity (by euglycemic hyperinsulinemic clamp), glucose tolerance (by standard glucose
tolerance test), lipid profile, renal hemodynamics (GFR and RPF by inulin and PAH renal
clearances, respectively), albuminuria (mean of three consecutive overnight urine
collections), albumin, IgG, Na+ and free water fractional clearances and other routine
laboratory analyses, patients satisfying the selection criteria will enter 4-month therapy
with rosiglitazone 4 mg/day, up-titrated, if well-tolerated, to 8 mg/day 4 weeks later.
Baseline evaluations will be repeated at the end of the treatment period and 2 months after
treatment withdrawal. Blood pressure, body weight and routine laboratory tests - including
liver function tests - will be evaluated also at 1 and 2 weeks of rosiglitazone therapy, at
month 1 and then every month up to study end. Albuminuria will also be evaluated at month 2
of rosiglitazone therapy.
No major change in diet and immunosuppressive, antihypertensive and other concomitant
treatments will be introduced throughout the whole study period. A low salt (2 grams of Na+
per day) and a controlled dietary protein intake (0.8 g/kg/body weight per day) will be
recommended to all patients. Should any evidence of clinically relevant water retention or
of liver toxicity occur throughout the treatment period, rosiglitazone will be back-titrated
to the initial dose or withdrawn as deemed clinically appropriate.
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Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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