Introduction
Type 2 diabetes is a progressive disease, primarily characterised by beta cell failure [
1,
2]. This progression is manifested clinically by a deterioration in HbA
1c levels over time, despite lifestyle and increased pharmacological interventions. However, the rate at which diabetes progresses is highly variable between individuals. Some individuals have a rapid deterioration and advance to insulin therapy quickly, whereas others can be adequately treated with non-insulin glucose-lowering medication for in excess of 20 years. Gaining insight into why some individuals progress rapidly while others do not will enable a more stratified approach to the management of type 2 diabetes by identifying subgroups who may require different management depending on their likelihood of diabetes progression.
Previous studies have investigated factors associated with the rate of diabetes progression. However, these studies have only reported an outcome based on progression to glucose-lowering medications (i.e. time to initiation of non-insulin glucose-lowering medication, failure of monotherapy or time to insulin therapy) [
1,
3‐
9]. In these studies, younger age at diagnosis and insufficient beta cell function were consistently associated with faster progression of diabetes. The UK Prospective Diabetes Study (UKPDS) reported that the presence of positive GAD antibody (GADA) concentrations predicted an increased likelihood of requirement for insulin [
3]. Other less well established associations were female sex, low BMI (defined as <30 kg/m
2), weight gain, lower HDL-cholesterol and higher serum creatinine. In addition, we have previously reported that risk of progression, defined by a requirement for insulin treatment, is associated with normal weight or obesity (a U-shaped relationship), and higher triacylglycerol and lower HDL-cholesterol levels [
6].
The studies outlined rely on defining an endpoint, such as a glycaemic threshold or starting a new drug. These ‘time to failure’ approaches are problematic, particularly in the real world, where decisions to start a drug may be subject to prescriber or patient inertia, or where fluctuations in HbA
1c, for example due to lifestyle change resulting from life or health status events, can trigger a failure event. A ‘coefficient of failure’ measure has been proposed to avoid these difficulties—in essence, deriving a rate of glycaemic deterioration for each individual [
10]. This approach was applied to the UKPDS study, which reported a coefficient of failure of 3.7 mmol/mol (0.34%) per year with chlorpropamide treatment [
10], and to the A Diabetes Outcome Progression Trial (ADOPT) study, which described a rate of glycaemic deterioration of 1.5 mmol/mol (0.14%) HbA
1c per year in the metformin monotherapy arm [
11]. However, to our knowledge, no studies have been reported describing the coefficient of failure in settings outside these clinical trials of monotherapy. Determining rates of deterioration in a population over time is challenging as underlying disease severity reflects not only observed HbA
1c, but also lifestyle and pharmacological interventions.
The aim of this study was to derive a model for the rate of deterioration of type 2 diabetes (coefficient of failure) in a large population-based cohort and to investigate the clinical, pharmacological, biochemical and immunological characteristics associated with fast and slow rates of glycaemic deterioration.
Methods
An observational cohort study was performed using comprehensive electronic medical records from individuals in the Genetics of Diabetes Audit and Research in Tayside Study (GoDARTS) database, which has previously been described elsewhere [
12,
13]. In short, this contains detailed information on all encashed prescriptions from 1994 onwards in Tayside, Scotland, as well as all biochemistry and BMI measures. Therefore, for each individual we have a comprehensive longitudinal record of diabetes therapy and glycaemic control.
The GoDARTS study was approved by the Tayside Committee on Medical Research Ethics, and informed consent was obtained from all participants (REC reference 053/04). The GoDARTS cohort and the research question outlined here were studied as part of the Diabetes Research on Patient Stratification (DIRECT) study, an EU Seventh Framework Programme (FP7) Innovative Medicines Initiative (see
www.direct-diabetes.org) project.
Statistical analysis
A linear mixed effects model was fitted. As the time intervals between HbA1c measurements were more or less unique to each individual, the ‘continuous time/continuous space’ spatial data covariance structure provided within the PROC MIXED procedure in SAS 9.4 (SAS Institute, Cary, NC, USA) was used to describe the covariance structure among the errors.
We began by fitting a model with both a fixed and random intercept and slope, and adjustment for non-insulin glucose-lowering drugs, glucocorticoid use and changes in BMI over time, fitted as fixed effects. The Studentised residuals were examined and any HbA1c measures >3 SD from the mean were removed as these values were considered likely to be outliers for that individual.
We then ran the model again for type 2 diabetes and GADA-positive individuals separately and compared the individual rates of glycaemic deterioration. These were calculated by adding together each individual’s random slope with the population average (fixed) slope.
The model was then expanded in individuals with type 2 diabetes only, owing to small numbers in the GADA-positive group, to include the baseline clinical covariates of interest. To model the effect of each covariate on glycaemic deterioration, an interaction term between the covariate and time was included. We fitted univariate models in which baseline covariates were added singly, and a multivariate model that included all univariately significant covariates together. Age at diagnosis was split into four age bands (<50, 50–<60, 60–<70 and ≥70 years), and BMI was split into five categories based on WHO definitions (<25, 25–<30, 30–<35, 35–<40 and ≥40 kg/m2). HDL-cholesterol and triacylglycerol concentrations were split into four clinically meaningful bands (HDL-cholesterol: <1, 1–<1.2, 1.2–<1.4 and ≥1.4 mmol/l; triacylglycerols: <1.5, 1.5–<2.5, 2.5–<3.5 and ≥3.5 mmol/l), with an additional ‘missing’ group created to avoid excluding individuals with missing values from the multivariate model. Calendar year of diagnosis was divided into quartiles.
All analyses were performed using SAS, and p < 0.05 was considered statistically significant in all analyses.
Discussion
In this large, observational, population-based study with a maximum follow-up period of over 20 years, we have applied a novel approach to modelling the progression of diabetes. We have shown that, in a real-world setting, the underlying mean coefficient of failure (rate of glycaemic deterioration) in individuals with type 2 diabetes is 1.4 mmol/mol (0.12%) HbA1c per year, and in GADA-positive individuals it is faster, with a mean rate of 2.8 mmol/mol (0.25%) per year. Furthermore, our results suggest that individuals with type 2 diabetes who deteriorate the fastest are those diagnosed under 50 years old, and that there is very limited deterioration in those diagnosed over the age of 70.
We report a coefficient of failure in individuals with type 2 diabetes comparable to that of the ADOPT clinical trial, which reported a 1.5 mmol/mol (0.14%) annual rate of deterioration in HbA
1c in a metformin monotherapy cohort [
11]. Moreover, we know from the UKPDS that GADA positivity is a strong predictor of diabetes progression [
3], and here we have shown that GADA-positive individuals progress approximately two times faster than individuals with type 2 diabetes. In the group of individuals who are not known to be GADA-positive, faster diabetes progression is associated with clinically small but statistically significant differences in BMI and HDL-cholesterol, in keeping with the insulin resistance phenotype.
Our findings are in accordance with other studies that have reported the association between younger age at diagnosis and faster progression of diabetes [
1,
4‐
8]. Individuals diagnosed younger than 50 years of age progress rapidly compared with individuals diagnosed over the age of 70 (Fig.
2), and as HbA
1c at diagnosis is higher in the younger than the older group (mean [95% CI]: 66.4 [65.1, 67.8] vs 61.9 [60.8, 62.9] mmol/mol; 8.23% [8.11%, 8.35%] vs 7.81% [7.71%, 7.90%];
p < 0.0001), this suggests that individuals diagnosed younger may benefit from being treated more aggressively with earlier initiation of glucose-lowering medications, particularly if future therapies can be established to delay progression. The finding that, in the real world, 66% of individuals with type 2 diabetes diagnosed after the age of 70 years progress at a rate <1.1 mmol/mol (0.1%) per year, and that only 1.5% progress at a rate >4.4 mmol/mol (0.4%) per year, is striking and highlights how glycaemic monitoring and management in those diagnosed at over 70 years may not need to be as aggressive as those diagnosed under 50 years of age.
We have previously reported that earlier calendar year of diagnosis is associated with risk of progression, as defined by requirement for insulin treatment [
6]. We believe that this reflects a change in practice over time, with possibly two factors influencing progression rate. First, individuals may be diagnosed earlier in more recent years due to screening or increased awareness. This is supported by the observation that individuals diagnosed prior to 2001 have a higher HbA
1c at diagnosis than those diagnosed in or after 2006 (mean [95% CI]: 65.1 [64.1, 66.0] vs 60.5 [59.5, 61.6] mmol/mol; 8.11% [8.02%, 8.20%] vs 7.68% [7.58%, 7.78%];
p < 0.0001). Second, with increasing calendar years, there may be improved general health and better treatment of all diabetes risk factors that may impact on rates of progression.
In this analysis, we included a group who at diagnosis had a high HbA1c of >64 mmol/mol (8%) but whose HbA1c level fell to meet the inclusion criteria within the first year. Many mechanisms may underlie this pattern, but one possible explanation is that these are a group who initially present with high HbA1c driven by gluco-lipotoxcity, who subsequently show rapid improvement with dietary and drug treatment. It is interesting to note that, in the multivariate analysis, this group, despite an initial high HbA1c, subsequently progressed at the same rate as those whose initial HbA1c was <64 mmol/mol (8%).
The aim of this study was to derive a ‘rate of deterioration’ or ‘coefficient of failure’, which we believe has many advantages over a time to failure model. However, a number of assumptions have been made in order to develop this model. First, we assume a linear deterioration in HbA
1c; this is supported by the Belfast Diet Study, which reported two linear phases before and after the diagnosis of diabetes [
1]. However, there may be individuals who do not follow this linear decline who are not well accounted for in our model. Second, individuals were excluded from entry into the model largely because they had a high HbA
1c at diagnosis that did not fall below 64 mmol/mol (8%) within the first year, or because they had too few HbA
1c measures before they progressed onto insulin. As such, our model excludes those with the most aggressive disease and/or those who present late with a high HbA
1c, and focuses on those diagnosed close to onset of diabetes or with less aggressive disease. Therefore our coefficients of failure are likely to underestimate the true progression rate in the population. Third, we define diabetes diagnosis as a first HbA
1c ≥48 mmol/mol (6.5%) following a clinical diagnosis of type 2 diabetes, and as an individual may have a diagnostic glucose level but an HbA
1c <48 mmol/mol (6.5%), this means that we will underestimate the duration of diabetes and overestimate the slope in some individuals. Finally, the fact that we are studying real-world individuals in clinical practice means that we lack some key measures that may be important for glycaemic deterioration, such as measures of beta cell function and insulin resistance.
In summary, we have developed a novel approach to model the coefficient of failure in observational data across multiple drug combinations. This approach may be valuable in investigating biomarker or genomic determinants of diabetes progression in bioresources. In addition, although our current model derives a ‘global’ rate of deterioration from diagnosis to insulin initiation, future developments may allow investigation of how the rate varies for therapies for diabetes and for other conditions. We confirm that GADAs are associated with greater glycaemic deterioration, and for the first time quantify the rate of glycaemic deterioration in the elderly. Our findings of minimal glycaemic deterioration in this elderly-onset group has important implications for stratifying diabetes care, suggesting that less intensive glycaemic monitoring and management is required for this group.
Acknowledgements
We acknowledge the support of the Health Informatics Centre, University of Dundee for managing and supplying the anonymised data. We are grateful to all the participants who took part in the GoDARTS study, to the general practitioners, to the Scottish School of Primary Care for their help in recruiting the participants, and to the whole team, which includes interviewers, computer and laboratory technicians, clerical workers, research scientists, volunteers, managers, receptionists and nurses. The Wellcome Trust provides support for Wellcome Trust United Kingdom Type 2 Diabetes Case Control Collection (GoDARTS), and informatics support is provided by the Chief Scientist Office. Some of the data were presented as an abstract at the EASD Annual Meeting in Vienna, 2014.