Relationship between glycaemic variability and hyperglycaemic clamp-derived functional variables in (impending) type 1 diabetes

Annelien Van Dalem; Simke Demeester; Eric V Balti; Katelijn Decochez; Ilse Weets; Evy Vandemeulebroucke; Ursule Van de Velde; An Walgraeve; Nicole Seret; Christophe De Block; Johannes Ruige; Pieter Gillard; Bart Keymeulen; Daniel G Pipeleers; Frans K Gorus; Belgian Diabetes Registry

doi:10.1007/s00125-015-3761-y

Relationship between glycaemic variability and hyperglycaemic clamp-derived functional variables in (impending) type 1 diabetes

Diabetologia. 2015 Dec;58(12):2753-64. doi: 10.1007/s00125-015-3761-y. Epub 2015 Sep 26.

Authors

Annelien Van Dalem¹, Simke Demeester¹, Eric V Balti¹, Katelijn Decochez¹, Ilse Weets^{2

3}, Evy Vandemeulebroucke¹, Ursule Van de Velde^{1

4}, An Walgraeve¹, Nicole Seret⁵, Christophe De Block⁶, Johannes Ruige⁷, Pieter Gillard^{1

8}, Bart Keymeulen^{1

4}, Daniel G Pipeleers¹, Frans K Gorus^{1

9}; Belgian Diabetes Registry

Collaborators

Belgian Diabetes Registry:
V Baeten, A de Brabanter, T De Mesmaeker, H Dewinter, N Diependaele, S Exterbille, T Glorieux, P Goubert, C Groven, T Haulet, A Ivens, D Kesler, F Lebleu, E Quartier, G Schoonjans, M Van Molle, S Vanderstraeten, L Van Gaal, R Braspenning, J Michiels, P Aerts, T De Mesmaeker, S Exterbille, P Goubert, C Groven, V Kemels, C Tettelin, S Vanderstraeten, A Walgraeve, J M Kaufman, A Hutse, A Rawoens, N Steyaert, S Deneve, N Platteau, C Mathieu, M Carpentier, M Robijn, K Rouffé, A Schoonis, H Morobé, S Achten, R Van Heyste, A Arrieta, K Casteels, C Mathieu, P Gillard, L Crenier, J De Schepper, I Gies, B Keymeulen, J Vanbesien, I Weets, K Decochez, E Vandemeulebroucke, C De Block, L Van Gaal, G Lamberigts, G Massa, A Messaaoui, T Mouraux, A Nollet, D Rocour-Brumioul, A Scheen, N Seret, G T'Sjoen, S Van Aken, A Verhaegen, E Weber

Affiliations

¹ Diabetes Research Center, Vrije Universiteit Brussel, Laarbeeklaan 100, 1090, Brussels, Belgium.
² Diabetes Research Center, Vrije Universiteit Brussel, Laarbeeklaan 100, 1090, Brussels, Belgium. [email protected].
³ Department of Clinical Chemistry and Radio-immunology, University Hospital Brussels, Brussels, Belgium. [email protected].
⁴ Department of Diabetology, University Hospital Brussels, Brussels, Belgium.
⁵ CHC Clinique de L'Espérance, Montegnée, Belgium.
⁶ Department of Endocrinology, Diabetology and Metabolism, University Hospital Antwerp, Antwerp, Belgium.
⁷ Department of Endocrinology, University Hospital Ghent, Ghent, Belgium.
⁸ Department of Endocrinology, University Hospital Leuven, Leuven, Belgium.
⁹ Department of Clinical Chemistry and Radio-immunology, University Hospital Brussels, Brussels, Belgium.

PMID: 26409458
DOI: 10.1007/s00125-015-3761-y

Abstract

Aims/hypothesis: We examined whether measures of glycaemic variability (GV), assessed by continuous glucose monitoring (CGM) and self-monitoring of blood glucose (SMBG), can complement or replace measures of beta cell function and insulin action in detecting the progression of preclinical disease to type 1 diabetes.

Methods: Twenty-two autoantibody-positive (autoAb(+)) first-degree relatives (FDRs) of patients with type 1 diabetes who were themselves at high 5-year risk (50%) for type 1 diabetes underwent CGM, a hyperglycaemic clamp test and OGTT, and were followed for up to 31 months. Clamp variables were used to estimate beta cell function (first-phase [AUC5-10 min] and second-phase [AUC120-150 min] C-peptide release) combined with insulin resistance (glucose disposal rate; M 120-150 min). Age-matched healthy volunteers (n = 20) and individuals with recent-onset type 1 diabetes (n = 9) served as control groups.

Results: In autoAb(+) FDRs, M 120-150 min below the 10th percentile (P10) of controls achieved 86% diagnostic efficiency in discriminating between normoglycaemic FDRs and individuals with (impending) dysglycaemia. M 120-150 min outperformed AUC5-10 min and AUC120-150 min C-peptide below P10 of controls, which were only 59-68% effective. Among GV variables, CGM above the reference range was better at detecting (impending) dysglycaemia than elevated SMBG (77-82% vs 73% efficiency). Combined CGM measures were equally efficient as M 120-150 min (86%). Daytime GV variables were inversely correlated with clamp variables, and more strongly with M 120-150 min than with AUC5-10 min or AUC120-150 min C-peptide.

Conclusions/interpretation: CGM-derived GV and the glucose disposal rate, reflecting both insulin secretion and action, outperformed SMBG and first- or second-phase AUC C-peptide in identifying FDRs with (impending) dysglycaemia or diabetes. Our results indicate the feasibility of developing minimally invasive CGM-based criteria for close metabolic monitoring and as outcome measures in trials.

Keywords: Beta cell function; Continuous glucose monitoring; Hyperglycaemic clamp; Insulin resistance; Prediabetes; Prediction; Prevention; Self-monitoring of blood glucose; Type 1 diabetes.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Adult
Area Under Curve
Blood Glucose / analysis*
Blood Glucose Self-Monitoring
C-Peptide / blood
Child
Diabetes Mellitus, Type 1 / blood*
Female
Glucose Clamp Technique*
Glucose Tolerance Test
Glycated Hemoglobin / analysis
Healthy Volunteers
Humans
Hyperglycemia / blood*
Insulin-Secreting Cells / metabolism
Male
Young Adult

Substances

Blood Glucose
C-Peptide
Glycated Hemoglobin A