Post-glucose-load urinary C-peptide and glucose concentration obtained during OGTT do not affect oral minimal model-based plasma indices

Post-glucose-load urinary C-peptide and glucose concentration obtained during OGTT do not affect oral minimal model-based plasma indices

The purpose of this study was to investigate how renal loss of both C-peptide and glucose during oral glucose tolerance test (OGTT) relate to and affect plasma-derived oral minimal model (OMM) indices. All individuals were recruited during family screening between August 2007 and January 2011 and un...

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Bibliographic Details
Published in:Endocrine Vol. 52; no. 2; pp. 253 - 262
Main Authors: Jainandunsing, Sjaam, Wattimena, J. L. Darcos, Rietveld, Trinet, van Miert, Joram N. I., Sijbrands, Eric J. G., de Rooij, Felix W. M.
Format: Journal Article
Language:English
Published: New York Springer US 01-05-2016
Subjects:
Adult
Biomarkers - urine
C-Peptide - urine
Diabetes
Diabetes Mellitus, Type 2 - urine
Endocrinology
Female
Glomerular Filtration Rate
Glucose Tolerance Test
Glycosuria
Humanities and Social Sciences
Humans
Internal Medicine
Male
Medicine
Medicine & Public Health
Middle Aged
Models, Biological
multidisciplinary
Original
Original Article
ROC Curve
Science
Type 2 diabetes
Oral minimal model
Glucose
South Asian
OGTT
C-peptide
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Summary:The purpose of this study was to investigate how renal loss of both C-peptide and glucose during oral glucose tolerance test (OGTT) relate to and affect plasma-derived oral minimal model (OMM) indices. All individuals were recruited during family screening between August 2007 and January 2011 and underwent a 3.5-h OGTT, collecting nine plasma samples and urine during OGTT. We obtained the following three subgroups: normoglycemic, at risk, and T2D. We recruited South Asian and Caucasian families, and we report separate analyses if differences occurred. Plasma glucose, insulin, and C-peptide concentrations were analyzed as AUCs during OGTT, OMM estimate of renal C-peptide secretion, and OMM beta-cell and insulin sensitivity indices were calculated to obtain disposition indices. Post-glucose load glucose and C-peptide in urine were measured and related to plasma-based indices. Urinary glucose corresponded well with plasma glucose AUC (Cau r  = 0.64, P  < 0.01; SA r  = 0.69, P  < 0.01), S I (Cau r  = −0.51, P  < 0.01; SA r  = −0.41, P  < 0.01), Φ dynamic (Cau r  = −0.41, P  < 0.01; SA r  = −0.57, P  < 0.01), and Φ oral (Cau r  = −0.61, P  < 0.01; SA r  = −0.73, P  < 0.01). Urinary C-peptide corresponded well to plasma C-peptide AUC (Cau r  = 0.45, P  < 0.01; SA r  = 0.33, P  < 0.05) and OMM estimate of renal C-peptide secretion ( r  = 0.42, P  < 0.01). In general, glucose excretion plasma threshold for the presence of glucose in urine was ~10–10.5 mmol L −1 in non-T2D individuals, but not measurable in T2D individuals. Renal glucose secretion during OGTT did not influence OMM indices in general nor in T2D patients (renal clearance range 0–2.1 %, with median 0.2 % of plasma glucose AUC). C-indices of urinary glucose to detect various stages of glucose intolerance were excellent (Cau 0.83–0.98; SA 0.75–0.89). The limited role of renal glucose secretion validates the neglecting of urinary glucose secretion in kinetic models of glucose homeostasis using plasma glucose concentrations. Both C-peptide and glucose in urine collected during OGTT might be used as non-invasive measures for endogenous insulin secretion and glucose tolerance state.
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ISSN:1355-008X
1559-0100
DOI:10.1007/s12020-015-0765-9