Insulin Resistance Clinical Trial
Official title:
Effects of Regular Protein Diet Supplemented With Keto Acid on Insulin Resistance In Peritoneal Dialysis Patients
The overarching aim of this proposal is to examine the effects of usual protein diet supplemented with keto acid (KA) on insulin sensitivity in patients on peritoneal dialysis (PD). The investigators will achieve this goal through a randomized controlled trial of administration of usual protein diet plus KA versus usual protein diet alone in patients on peritoneal dialysis (PD) over a period of 6 months. If successful, the results of this study will provide potential avenues for improvement of metabolic profile of patients on PD and possibly improve long-term outcomes such as cardiovascular disease risk and death.
Specific Aims and Significance:
To evaluate the effects of KA plus usual protein diet on basal and stimulated insulin
sensitivity in PD patients.
Hypothesis: Administration of KA plus usual protein diet will improve insulin resistance in
peritoneal dialysis patients.
To evaluate the influence of KA plus usual protein diet on non-traditional cardiovascular
disease (CVD) markers (markers of inflammation and oxidative stress) in PD patients.
Hypothesis: Administration of KA plus usual protein diet will improve markers of
inflammation and oxidative stress in PD patients.
Background and Rationale:
Insulin Resistance in Peritoneal Dialysis Patients. Insulin resistance (IR), the reciprocal
of insulin sensitivity, describes a state of reduced biological effect for any given
concentration of insulin in the plasma. Insulin resistance plays a major pathophysiological
role in glucose intolerance and Type 2 diabetes mellitus (T2DM) and is tightly associated
with major public health problems including obesity, hypertension, dyslipidemia, and
atherosclerotic cardiovascular disease. Insulin resistance, measured by homeostatic model
assessment (HOMA-IR), is reported to be common in chronic kidney disease (CKD) patients,
including ones on PD and hemodialysis (HD). HOMA-IR is also shown to be an independent
predictor of cardiovascular mortality in non-diabetic maintenance HD patients although the
pathophysiological link has not been clearly delineated.
A unique aspect of PD that predisposes patients to IR is the inevitable glucose load from
the dialysate required for ultrafiltration. Consequently, the prevalence of metabolic
syndrome such as hyperglycemia, dyslipidemia and weight gain is increased in PD patients. As
an individual component of metabolic syndrome, IR is significantly higher in PD patients
than in HD or pre-dialysis patients (47% vs 21% or 26%). Accordingly, improvement of IR
could be a potential intervention to decrease the CVD risk and mortality in PD patients.
However, only a few investigations have centered on interventions to ameliorate IR in these
patients.
Low Protein Diet Supplemented with Keto Acid as a Potential Strategy to Ameliorate Insulin
Resistance in PD Patients. Several small scale studies exploring the effects of low protein
diet (LPD) plus KA on glucose metabolism indicated that LPD-KA could improve liver and
peripheral tissue insulin sensitivity in CKD patients not yet on maintenance dialysis. There
are no studies exploring such effects in maintenance dialysis patients, especially in PD
patients. One potential mechanism for the improvement in insulin resistance by KA is the
reduction of circulating uremic toxins, although the specific elements are not well
delineated. In addition, the supplementation of KA might be helpful since plasma total
branched-chain amino acid concentrations correlate with glucose tolerance index in dialysis
patients. Since the safety of LPD has not been entirely shown in previous studies for PD
patients, and our data indicated that DPI < 0.74g/kg/d was harmful in the long-term PD, the
investigators will not provide the LPD for improving the IR. However, the exploration of
possible benefits of KA plus usual protein intake in PD patients on insulin sensitivity is
intriguing.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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