ESRD Clinical Trial
Official title:
Glucose Metabolism During Hemodialysis
Disturbed glucose metabolism is a common feature of patients with end-stage renal disease
(ESRD). Several hormones responsible of a stable blood glucose including insulin, glucagon,
and the gastrointestinal insulinotropic hormones Glucagon-like Peptide-1 (GLP-1) and
Glucose-dependent Insulinotropic Peptide (GIP) are elevated in patients with ESRD. These
hormones are all medium sized peptides which theoretically makes them removable during high
efficient hemodialysis. A significant removal could have consequences for the treatment of
patients with diabetes and ESRD.
The purpose of this study is to determine whether insulin, glucagon, GLP-1 and GIP are
cleared during high efficient hemodialysis and hemodiafiltration. The investigators
hypothesize that a significant amount of these hormones is removed during hemodialysis and
to a larger extend during hemodiafiltration.
BACKGROUND
Disturbed glucose metabolism is a common feature of patients with end-stage renal disease
(ESRD). Furthermore, the prevalence of diabetes mellitus in the ESRD population is high
resulting in a marked increased morbidity and mortality. Several hormones responsible of a
stable blood glucose including insulin, glucagon, and the gastrointestinal insulinotropic
hormones Glucagon-like Peptide-1 (GLP-1) and Glucose-dependent Insulinotropic Peptide (GIP)
are elevated and dysregulated in patients with ESRD. Newly developed antidiabetic
medications such as the dipeptidyl peptidase-4 inhibitors (DPP-4 inhibitors) increase the
concentrations of these hormones making the effect of these treatments difficult to predict
in patients with ESRD.
During the history of hemodialysis the treatment has been refined to increase the removal of
the various substances that accumulate when the kidney function declines. The focus has
primary been on the removal of smaller molecules such as creatinine and urea, but in recent
decades the focus has moved to medium-sized molecules (molecular weight of 300 to 12,000 Da)
which are suspected of causing various uremic complications such as amyloidosis and
neuropathy. The dialysis technique has therefore been optimized such that relatively large
molecules are removed, but the dialysis filter does not distinguish between wanted and
unwanted substances. Thus, in contrast to the functioning kidney there is a risk of removing
important molecules including hormones, which are essential for maintaining a normal glucose
metabolism.
Insulin, glucagon and the incretin hormones, GLP-1 and GIP are all peptides with a molecular
weight of 3300 to 5800 Da. This means that they theoretically have a size where they can be
removed under hemodialysis with so-called high-flux filters and by hemodiafiltration, both
of which are common standards of care for patients with ESRD. It has been shown that insulin
is removed in significant quantities during a hemodialysis, but this is probably due to
adsorption to the filter and not filtration. Whether glucagon and the incretin hormones are
eliminated by high effective hemodialysis and hemodiafiltration is never investigated.
Previous studies have primarily observed unchanged glucagon and GIP concentrations in the
blood after conventional hemodialysis. One study showed a 30% decrease in GIP concentration
after hemodialysis, but the detected change probably reflects altered metabolism due to the
treatment as the dialysis technique at the time was too inefficient to remove peptides
significantly. Assays for the analysis of incretin hormones have also become considerably
more specific and now differentiate between the active hormones and their inactive
intermediate metabolites.
In recent years there has been a growing development of drugs that increase the endogenous
produced incretin hormones. Linagliptin, launched in 2011, is the only one that is approved
for patients with ESRD since it is not cleared renally and therefore does not require a
change in dosage. However, the elimination of incretin hormones in dialysis patients is
sparingly studied both during and between dialysis treatments.
This study will determine the effect of high efficient dialysis treatment on a number of
hormones regulating the blood glucose. Significant elimination of these hormones during
dialysis can have therapeutic implications for the treatment of dialysis patients with
incretin based therapies.
PURPOSE OF THE STUDY
The purpose of this study is to determine whether several blood glucose-regulating hormones
and their metabolites are removed during hemodialysis and hemodiafiltration in patients with
dialysis-dependent renal insufficiency. The hypothesis is that the dialysis treatment
results in a significant removal, thereby reducing the plasma concentration of each hormone.
METHODS
10 patients with ESRD undergoing either chronic hemodialysis or chronic hemodiafiltration
will be included. The study will be carried out on two separate days which are planned two
days after their previous dialysis. On the two study days each participant will be treated
with a 4 hour hemodialysis or hemodiafiltration. Besides the dialysis modality (hemodialysis
and hemodiafiltration) the two study days will be alike.
The participant will be examined in the morning in a 10 hour fasting state (including
smoking) without any alcohol consumption within the last 24 hours and strenuous physical
activity within the last 2 hours. Weight, Height, blood pressure and pulse will be measured
and the dialysis access is prepared. An initial blood sample will be analyzed immediately
for sodium, bicarbonate and ionized calcium and the dialysate of the dialyzer will be
adjusted to match the measured concentrations as close as possible. The ultrafiltration will
be set according to the patients dry weight and no sodium or ultrafiltration profiles will
be allowed. The blood flow will be held constant not exceeding the half of the flow of the
arteriovenous fistula.
Each participant at each study day will receive the dialysis fasting for one hour after
which a standardized liquid meal with 1.5 mg Paracetamol added will be administered.
During the dialysis blood samples will be measured repeatedly and analyzed for insulin,
glucagon, GLP-1 and GIP. Blood samples will be drawn both before and after the dialysis
filter to calculate the clearance and samples from the spend dialysate are collected to
determine the amount of adsorption of the hormones to the dialysis filter.
Participants undergo an optional third examination day receiving the standardized meal test
without dialysis. Blood samples are collected at the same time intervals as during the
examination days with dialysis.
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Observational Model: Case-Only, Time Perspective: Prospective
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