Diabetes Mellitus Clinical Trial
Official title:
B-type Natriuretic Peptide Affects the Initial Response to Intravenous Glucose in a Placebo-controlled Cross-over Study in Healthy Volunteers
Rationale: B type natriuretic peptide (BNP) is a hormone released from cardiomyocytes in
response to myocyte stretching and serves as a reliable biomarker in the diagnosis of
cardiac dysfunction and heart failure. Recent observations speak for a distinct connection
between chronic heart failure and diabetes mellitus.
Objective: The study was set out to investigate the role of BNP on parameters of glucose
metabolism in a placebo controlled cross-over study in healthy volunteers.
Methods and Results: Ten participants (25±1 years; BMI 23±1 kg/m2; fasting glucose 83±2
mg/dL) received either placebo or 3 pmol/kg/min BNP 32 intravenously for 4h. One hour after
beginning the BNP/placebo infusion, a 3h intravenous glucose tolerance test (0.33 g/kg
glucose + 0.03 U/kg insulin at 20 min) was performed and plasma glucose, insulin and C
peptide were frequently measured. BNP increased the initial glucose distribution volume
(13±1 %BW vs. 11±1, P<0.002), leading to an overall reduction of glucose concentration
(P<0.001) especially during the initial 20 min of the test (P=0.001), accompanied by a
reduction of the initial C peptide levels (4.3±0.4 ng/mL vs. 4.9±0.3, P=0.015). BNP had no
impact on beta cell function, insulin clearance or insulin sensitivity.
Discussion: Intravenous administration of BNP increases glucose initial distribution volume
and lowers plasma glucose concentrations after a glucose load without affecting beta cell
function or insulin sensitivity what speaks for the concept that BNP is not diabetogenic,
but improves the metabolic status in patients with heart failure. This opens new questions
regarding BNP induced differences in glucose availability and signalling in several
organs/tissues.
In one of our recent studies we investigated insulin sensitivity (OGIS index) and insulin
secretion (beta cell function with the insulinogenic index, IGI) in patients with heart
insufficiency by frequently sampled oral glucose tolerance test (21). Insulin sensitivity
was impaired in CHF compared to control (OGIS: 354±14 ml/min/m2 vs. 450±20; p<0.003). Also
beta cell function was reduced (IGI: 100±14 vs. 150±45 pmolINS/pmolGLUC). Interestingly a
significant inverse correlation exists between BNP and IGI (r=0.41, p<0.05) (21). The
relationship between BNP and glucose metabolism has only been partially investigated. Plasma
BNP rises in response to hyperglycemia, but is not influenced by hyperinsulinemia (22, 23).
On the other side, the physiological role of BNP on beta cell function and insulin
sensitivity has not been investigated to date. As BNP levels rise with the degree of heart
insufficiency and insulin resistance correlates to the degree of cardiomyopathy, we
hypothesize that BNP influences glucose metabolism in healthy men.
One gold standard investigation of both beta cell function and peripheral insulin
sensitivity is the insulin-modified frequently sampled intravenous glucose tolerance test
(FSIGT). The FSIGT consists in giving intravenously a glucose bolus at time point 0 followed
by an intravenous administration of insulin at time point 20 minutes (18,19, 20). The
determination of glucose, insulin and C-peptide at frequent intervals till time point 180
minutes allows the calculation of the acute insulin response, glucose effectiveness, insulin
clearance and insulin sensitivity through the minimal model analysis (13) The intravenous
administration of 3 pmol/kg/min BNP achieves a plateau of increased BNP plasma
concentrations after 60 minutes. In previous publications, this infusion was administered
during 4 hours, achieving a steady state plasma BNP between time points 60 minutes and 240
minutes (17). Using this already established protocol, we aim to maintain constantly high
plasma BNP levels throughout the three hours of the FSIGT. The combination of both BNP (17)
and FSIGT (13) protocols in an interventional study will be an adequate means of
investigating the impact of BNP on glucose metabolism in healthy subjects.
The present study aims to investigate the effect of intravenous infusion of BNP-32 (American
Peptide, Calif., US) on the beta cell function and insulin sensitivity during FSIGT in
healthy volunteers.
-65, -60, -30, 0, 3, 4, 5, 6, 8, 10, 14, 19, 22, 27, 30, 35, 40, 50, 60, 70, 90, 100, 120,
140, 150 and 180 min for the measurement of glucose, insulin and C-peptide (8 ml per time
point: time points -30, 0, 3, 4, 5, 6, 8, 10, 14, 19, 22, 27, 30, 35, 40, 50, 70, 100, 140
and 180 min), for the measurement of BNP and NT-proBNP (4 ml per time point: time points
-65, -60, -30, 0, 30, 60, 90, 120, 150 and 180 min) and for the measurement of plasma
sodium, potassium and creatinine (8 ml per time point: time points -60, 60 and 180 minutes).
Primary outcome parameter is area under the curve of insulin (AUCinsulin) from time point
-30 to 180 min.
Secondary outcome parameters are AUCglucose and AUCc-peptide from time point -30 to 180 min,
BNP- and NT-proBNP levels from time point -65 to 180, plasma sodium, potassium and
creatinine from time point -60 to 180.
On study days volunteers will come to the study room at around 07:45 a.m. after an overnight
fasting. After being weighed, they will remain in bed throughout the study, except when
standing to pass urine. Two vein flow needles (Venflon, Helsingborg, Sweden) will be
inserted in the antecubital veins of the right and left arm for the administration of
infusions and blood sampling respectively. The subjects will rest for approximately 15
minutes before obtaining baseline blood samples (at time point - 65 minutes).
3.0 pmol/kg/min human BNP-32 (American Peptide, Calif., US) which is solved in Haemaccel (10
mL/h), or placebo (Haemaccel, 10 mL/h, alone) will be continuously administered for 4 hours,
between time points -60 and 180 minutes, using a syringe pump (Treonic, Vickers Medical,
Basingstoke, United Kingdom). A washout period of at least 2 weeks will be between the
administration of BNP and placebo on the two different study days. This protocol has been
used in the study of Lainchbury et al. (17).
330 mg/kg body weight glucose will be administered as a bolus during 30 seconds at time
point 0-0.5 minutes.
0.03 IU/kg rapidly acting insulin (Actrapid, Novo-Nordisk, Denmark) will be infused
intravenously for 5 minutes starting at time point 20.
Blood samples will be collected at time points: -65, -60, -30, 0, 3, 4, 5, 6, 8, 10, 14, 19,
22, 27, 30, 35, 40, 50, 60, 70, 90, 100, 120, 140, 150 and 180 min for the measurement of
glucose, insulin and C-peptide (8 ml per time point: time points -30, 0, 3, 4, 5, 6, 8, 10,
14, 19, 22, 27, 30, 35, 40, 50, 70, 100, 140 and 180 min), for the measurement of BNP and
NT-proBNP (4 ml per time point: time points -65, -60, -30, 0, 30, 60, 90, 120, 150 and 180
min) and for the measurement of plasma sodium, potassium and creatinine (8 ml per time
point: time points -60, 60 and 180 minutes).
A final safety blood sample will be collected at time point 270 min for plasma sodium,
potassium, creatinine and BNP, NT-proBNP, sodium, potassium, creatinine, GPT, gamma-GT,
total bilirubin to ensure that (NT-pro)BNP levels returned to baseline and other parameters
are within the normal range.
Total volume of blood withdrawal will be about 230 ml. When voiding, the subjects will be
asked to collect the urine excreted during the study period (-65 till 180 minutes). for the
measurement of sodium, potassium and creatinine excretion.
Heart rate and blood pressure will be continuously monitored during the whole study. If the
systolic blood pressure is lower than 85 mmHg or the heart rate is less than 50 beats per
minute BNP infusion will be stopped.
Data analysis for estimating insulin sensitivity, ß-cell secretion, insulin clearance,
insulin hepatic extraction and insulin appearance rate will be done by minimal model
computer analysis of the frequently sampled intravenous glucose tolerance test
;
Allocation: Randomized, Intervention Model: Crossover Assignment, Masking: Single Blind (Subject), Primary Purpose: Basic Science
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