The Effect of Glucose Variability on the Risk of Microvascular Complications in Type 1 Diabetes: Response to Kilpatrick et al.

doi:10.2337/dc06-1594

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Letters: Comments and Responses

The Effect of Glucose Variability on the Risk of Microvascular Complications in Type 1 Diabetes

Response to Kilpatrick et al.

Louis Monnier, MD¹, Claude Colette, PHD², Lawrence Leiter, MD³, Antonio Ceriello, MD⁴, Markolf Hanefeld, MD⁵, David Owens, MD⁶, Naoko Tajima, MD⁷, Jaakko Tuomiletho, MD⁸, Jaime Davidson, MD⁹ On Behalf of the PGR Group

¹ Department of Metabolic Diseases, University Hospital of Montpellier, Montpellier, France
² Laboratory of Human Nutrition and Atherogenesis, University Institute of Clinical Research, Montpellier, France
³ Department of Nutritional Sciences, University of Toronto, Toronto, Canada
⁴ Clinical Sciences Research Institute, University of Warwick, Coventry, U.K.
⁵ Centre for Clinical Studies, Technical University of Dresden, Dresden, Germany
⁶ Academic Centre, Diabetes Research Unit, Llandough Hospital, Cardiff, U.K.
⁷ JIKEI University School of Medicine, Tokyo, Japan
⁸ National Public Health Institute, Helsinki Finland
⁹ University of Texas, Dallas, Texas

Address correspondence to Louis Monnier, MD, Lapeyronie Hospital, 34295 Montpellier Cedex 5, France. E-mail: l-monnier{at}chu-montpellier.fr

In an analysis of the datasets collected in the Diabetes Controland Complications Trial, Kilpatrick et al. (1) reported thatmean blood glucose was predictive of microvascular complicationsin patients with type 1 diabetes, while glucose variabilitydid not appear to be a factor in their development. We questiontheir methodology and thereby also the conclusions. They calculatedthe variability of within-day blood glucose as the SD aroundthe mean of a seven-point glycemic profile measured at eachpatient’s quarterly visit. With such a methodology, theyhave probably not selected major glucose fluctuations, but rathera composite of both major and minor fluctuations, and most ofthem were likely to be minor. Furthermore, they have probablyblunted the contribution of major glucose fluctuations, as itis not likely that the four pre- and interprandial and threepostprandial glucose values included in the seven-point profilewere in perfect coincidence with the nadirs and peaks of glucose,respectively. In contrast, the mean amplitude of glycemic excursions(MAGE) described by Service et al. (2) are designed to quantifymajor swings of glycemia and to exclude minor ones, since itsmeasurement is obtained by calculating the differences betweenconsecutive peaks or nadirs and includes only those greaterthan the SD of mean glycemic values. Indirect evidence for thisis given by observations from the study of Monnier et al. (3).By further analyzing their data, they first found that the MAGEvalue in 21 patients with type 2 diabetes was much greater (75mg/dl) than the SDs of within-day blood glucose calculated fromseven-point glycemic profiles (37 mg/dl). Second, the activationof oxidative stress, as estimated from urinary excretion ratesof isoprostanes, was highly correlated with MAGE calculatedfrom continuous monitoring of glucose in the interstitial fluid(r = 0.85; P < 0.0001) (3). A deterioration of this relationship(r = 0.43; P = 0.05) was observed when SDs of seven-point glycemicprofiles were substituted for MAGE values.

Even though the MAGE determination requires continuous glucosemonitoring, we believe that this parameter should be the "goldstandard" for assessing glucose fluctuations in all prospectiveinterventional studies designed to estimate glucose variability.We therefore believe that additional studies are required todefinitively determine the role of glycemic variability in thepathogenesis of the micro- and macrovascular complications ofdiabetes. Even though the technology of continuous measurementsof glucose in interstitial fluid remains a subject of debate,the use of continuous glucose sensors might be useful for conductingsuch trials.

Footnotes

L.L. has received research funding from, has provided CME onbehalf of, and has acted as a consultant to Eli Lilly, GlaxoSmithKline,Novartis, Pfizer, and sanofi-aventis. M. H. has served on theboards of the following studies: GlaxoSmithKline RECORD, GlaxoSmithKline-DREAM,sanofi-aventis ORIGIN, and Novartis NAVIGATOR and has receivedhonoraria for lectures from Takeda, Sanyko, Bayer, GlaxoSmithKline,sanofi-aventis, and Merck Sharp & Dohme. J.D. has takenpart in research studies with Eli Lilly, sanofi-aventis, Novartis,SmithKline Beecham, and Novo Nordisk and has been a consultantand/or speaker for Kos, Bristol Myer Quibb, Eli Lilly, sanofi-aventis,Pfizer, SmithKline Beecham, Takeda, Novartis, and Roche.

References

Kilpatrick ES, Rigby AS, Atkin SL: The effect of glucose variability on the risk of microvascular complication in type 1 diabetes. Diabetes Care 29:1486–1490, 2006[Abstract/Free Full Text]
Service FJ, O’Brien PC, Rizza RA: Measurements of glucose control. Diabetes Care 10:225–237, 1987[Medline]
Monnier L, Mas E, Ginet C, Michel F, Villon L, Cristol JP, Colette C: Activation of oxidative stress by acute glucose fluctuations compared with sustained chronic hyperglycemia in patients with type 2 diabetes. JAMA 295:1681–1687, 2006[Abstract/Free Full Text]

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