Diabetes Care 31:927-929, 2008 DOI: 10.2337/dc07-1863 © 2008 by the American Diabetes Association
A1C in Children and Adolescents With Diabetes in Relation to Certain Clinical ParametersThe Swedish Childhood Diabetes Registry SWEDIABKIDS
1 Faculty of Health Sciences, Linköping University, Linköping, Sweden Corresponding author: Lena Hanberger, Division of Pediatrics, Faculty of Health Sciences, S-581 85 Linköping, Sweden. E-mail: lena.hanberger{at}lio.se
OBJECTIVE—We explored the relationship between A1C and insulin regimen, duration of diabetes, age, sex, and BMI as well as the differences between clinical mean A1C levels at pediatric diabetes clinics in Sweden. RESEARCH DESIGN AND METHODS—Data from 18,651 clinical outpatient visits (1,033 girls and 1,147 boys) at 20 pediatric clinics during 2001 and 2002 registered in the Swedish Childhood Diabetes Registry SWEDIABKIDS, a national quality registry, were analyzed.
RESULTS—A1C was <7.0% (target value CONCLUSIONS—Adolescents with a high insulin dose and a long duration of diabetes, especially girls, need to be focused on. Differences in mean values between centers remained inexplicable and require further investigation.
Good metabolic control in type 1 diabetes is crucial (1), but for unclear reasons A1C levels differ greatly between clinics (2). Therefore, we analyzed data from a national quality registry, the Swedish Childhood Diabetes Registry SWEDIABKIDS. Since 2000, all data from outpatient visits are registered locally in a specially designed program for childhood diabetes. Our analysis included each patient's 2-year mean values of A1C, insulin dose, number of insulin injection times per day, duration of diabetes, BMI, number of visits to outpatient clinics per patient-year, sex, and age. The study group consisted of patients <20 years of age (n = 3,195: 1,526 girls and 1,669 boys) registered during 2001 and 2002. Data from 18,651 registered visits (9,177 by girls and 9,474 by boys) were analyzed after excluding 363 incorrectly registered visits. When insulin dose was <0.5 units · kg–1 · day–1 and diabetes duration was <1 year (n = 682) or not reported (n = 333), subjects were excluded. Of the 42 pediatric departments in Sweden, 22 provided data to the register. Two centers, one reporting data from only one visit per patient and one not reporting insulin dose, were excluded.
The mean ± SD number of visits per patient-year was 2.9 ± 3.4 (range 1–14), after excluding one outlier. The number of patients per center varied from 57 to 474. A1C was measured with the DCA-2000 analyzer (Bayer Diagnostics) or with local laboratory methods. All methods are standardized through EQUALIS (External Quality Assurance in Laboratory Medicine in Sweden) and are traceable to the Mono S method. Swedish A1C values are
We used four categories of A1C, referring to different levels of care and clinical interventions at our department in Linköping: <7.0% (target value at the time of data collection), 7.0–7.9% (intensified adjustment of insulin dose, diet, and physical activities), 8.0–9.9% (visits to outpatient clinic once a month), and Statistical analysis was performed using SPSS, version 14.0. Descriptive statistics are expressed as mean ± SD or SEM where indicated. For comparisons between groups, t test was used, and for comparisons between multiple variables, ANOVA was used. For correlations, the Pearson correlation coefficient was calculated. Results were considered significant at P < 0.05. Multivariable linear regression analysis was used to identify significant independent correlates of A1C.
In the analyzed population (n = 2,180: 1,033 girls and 1,147 boys) the mean age was 13.4 ± 3.9 years (range 1.9–19.9); the proportion of overweight (age- and sex-adjusted BMI 25 kg/m2) and obese (age- and sex-adjusted BMI 30 kg/m2) children was 19.8 and 3.0%, respectively; the mean duration of diabetes was 6.0 ± 3.7 years (range 1.0–18.5); the mean insulin dose was 1.00 ± 0.27 units · kg–1 · day–1 (range 0.50–2.94); the mean number of times insulin was given per day was 4.5 ± 0.7 times per day (range 1–7.6); and the proportion of rapid-acting insulin was 49 ± 13% (range 6–100), after excluding one outlier.
Metabolic control
Centers Mean A1C varied between centers from 6.8% (95% CI 6.8–6.9) to 8.2% (8.1–8.3), P < 0.001. Adjusting for age, sex, duration of diabetes, insulin dose, age- and sex-adjusted BMI SD, number of injection times per day, and number of visits per patient-year, mean A1C varied between 6.5% (6.4–6.7) and 8.7% (8.4–8.9), P < 0.001. Of the 20 centers, only 1 reported a mean A1C below our target value (7.0%). The number of visits to the centers, mean insulin dose, and duration of diabetes did not correlate with the centers mean A1C. In a multiple regression model, significant predictors of increasing A1C were high insulin dose (β = 1.09, P < 0.001) followed by high numbers of visits per patient-year (β = 0.14, P < 0.001), long diabetes duration (β = 0.05, P < 0.001), and older age (β = 0.03, P < 0.001), most obviously in girls. The mean center A1C varied significantly (P < 0.001). The difference remained significant after adjusting for age, sex, duration of diabetes, insulin dose, age- and sex-adjusted BMI SD, number of injections per day, and number of visits per patient-year.
In Sweden, all pediatric clinics and one primary health care unit treat all children and adolescents with diabetes from defined geographic areas. We thus have data from an unselected population at each center. Clinics from Stockholm did not report data. Despite the modern treatment and care given by multidisciplinary teams, only 35% of the children and adolescents had A1C <7.0%. Poor glycemic control was associated with older age, high insulin dose, and long duration of diabetes (2), especially during adolescence, suggesting that circumstances during puberty, both physical and psychological, affect metabolic control. High insulin dose, number of visits per patient-year, and long duration of diabetes were the strongest predictors of high A1C level (6). We assume that it is common to prescribe an increased insulin dose when A1C is increasing. A1C increased by 0.045% for each year with diabetes. There were pronounced differences in mean A1C between centers. Differences in characteristics of the populations did not explain the differences in A1C. According to the Hvidøre study (7), diabetes education, attitudes of the diabetes team, and treatment target values may underlie center differences. More efforts are required to reduce A1C levels. The pronounced differences in A1C per center cannot be explained by differences in formal treatment.
The Swedish Childhood Diabetes Registry was financially supported by the Swedish Child Diabetes Foundation (Barndiabetesfonden) and the National Board of Health and Welfare. We thank statistician John Carstensen, the steering committee of SWEDIABKIDS (Bengt Lindblad [national coordinator], Leif Blom, Ragnar Hanås, Ulf Samuelsson, and Ingmar Zachrisson), and the local coordinators who provided data (Agne Lind, Borås; Inga-Lena Lödesjö, Eskilstuna; Bengt Lindblad, Göteborg; Nils-Östen Nilsson, Halmstad; Jan Neiderud, Helsingborg; Erik Carlsson, Kalmar; Gudrun Jonsell, Karlstad; Christer Gundewall, Kungsbacka; Bert Thrybom, Lidköping; Ulf Samuelsson, Linköping; Maria Nordwall, Norrköping; Lennart Hellenberg, Nyköping; Henrik Tollig, Skövde; Nils Wramner, Trollhättan; Ragnar Hanås, Uddevalla; Ingemar Svenne, Uppsala; Margareta Blomgren, Visby; Carl-Göran Arvidsson, Västerås; Stig Edvardsson, Växjö; Torsten Gadd, Ángelholm; and Carina Bodén, Östersund).
Published ahead of print at http://care.diabetesjournals.org on 30 January 2008. DOI: 10.2337/dc07-1863. The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C Section 1734 solely to indicate this fact. Received for publication September 23, 2007. Accepted for publication January 22, 2008.
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