Estimated glucose disposal rate and risk of stroke and mortality in type 2 diabetes: a nationwide cohort study

Background and aims

Insulin resistance contributes to the development of type 2 diabetes (T2D) and is also a cardiovascular risk factor. The aim of this study was to investigate the potential association between insulin resistance measured by estimated glucose disposal rate (eGDR) and risk of stroke and mortality thereof in people with T2D.

Materials and methods

Nationwide population based observational cohort study that included all T2D patients from the Swedish national diabetes registry between 2004 and 2016 with full data on eGDR and categorised as following: < 4, 4–6, 6–8, and ≥ 8 mg/kg/min. We calculated crude incidence rates and 95% confidence intervals (CIs) and used multiple Cox regression to estimate hazard ratios (HRs) to assess the association between the risk of stroke and death, according to the eGDR categories in which the lowest category < 4 (i.e., highest grade of insulin resistance), served as a reference. The relative importance attributed of each factor in the eGDR formula was measured by the R² (± SE) values calculating the explainable log-likelihoods in the Cox regression.

Results

A total of 104 697 T2D individuals, 44.5% women, mean age of 63 years, were included. During a median follow up-time of 5.6 years, 4201 strokes occurred (4.0%). After multivariate adjustment the HRs (95% CI) for stroke in patients with eGDR categories between 4–6, 6–8 and > 8 were: 0.77 (0.69–0.87), 0.68 (0.58–0.80) and 0.60 (0.48–0.76), compared to the reference < 4. Corresponding numbers for the risk of death were: 0.82 (0.70–0.94), 0.75 (0.64–0.88) and 0.68 (0.53–0.89). The attributed relative risk R² (± SE) for each variable in the eGDR formula and stroke was for: hypertension (0.045 ± 0.0024), HbA1c (0.013 ± 0.0014), and waist (0.006 ± 0.0009), respectively.

Conclusion

A low eGDR (a measure of insulin resistance) is associated with an increased risk of stroke and death in individuals with T2D. The relative attributed risk was most important for hypertension.

The prevalence of type 2 diabetes (T2D) is increasing worldwide with rising human suffering from morbidity and mortality [1]. People with T2D are at higher risk of cardiovascular disease compared to people without diabetes, and a high prevalence of atherosclerotic disease i.e., myocardial infarction, peripheral artery disease and stroke exists [2, 3].

Strong traditional risk factors such as hypertension and hyperlipidaemia explain some of the increased risk of stroke observed in people with T2D. Recently our group showed that people with T2D with poor glycaemic control were at higher risk for stroke compared with T2D people who were well controlled demonstrating the importance of glycaemic control and the association for stroke [4]. Insulin resistance, which is more or less obligate in T2D and often following hyperglycaemia, is also suggested to be a strong risk factor for cardiovascular disease [5]. Preventing insulin resistance would yield as much as 40% reduction in atherosclerotic disease regardless of other well known risk factors such as hypertension, hyperlipidaemia, hyperglycaemia or obesity, involved in the insulin resistance state [6].

Gold standard technique measuring insulin resistance is the euglycaemic hyperinsulinaemic clamp method [7]. However, it is invasive and costly and therefore not suitable for large-scale clinical use. For that reason, a method based on the readily available clinical factors waist circumference, hypertension, and glycosylated haemoglobin A1c (HbA1c) was developed to estimate glucose disposal rate (eGDR) in patients with type 1 diabetes [8]. This method is proven to have a high precision when compared to the euglycaemic hyperinsulinaemic clamp method, and therefore, an excellent tool to measure insulin resistance in a large patient population [9]. Recently, our and other groups have used eGDR as a proxy for insulin resistance to predict long-term outcomes also in people with T2D [10].

Whether grade of insulin resistance predicts stroke in people with T2D is not well known [11, 12]. We performed a nationwide population-based cohort study using the Swedish national diabetes register (NDR) to investigate the association between insulin resistance measured by eGDR and risk of first-time stroke and mortality thereof in people with T2D.

This was a nationwide registry based retrospective nationwide cohort study, approved by the regional ethics committee in Gothenburg, Sweden (EPN Dnr 776-14).

Study population and data sources

All adult individuals (≥ 18 years) with T2D between 2004 and 2016 were included, from the Swedish national diabetes register (NDR) [13]. T2D was defined as diabetes treated with diet or oral hypoglycaemic agents alone, or age of > 40 years at onset of diabetes and treatment with insulin alone, or in combination with oral hypoglycaemic agents [14].

Data from NDR was combined with; the in-patient registry (IPR) with nationwide data for primary and secondary discharge diagnoses [15], the causes of death register, and the longitudinal integration database for health insurance and job market studies (LISA; Statistics Sweden) for socioeconomic data [16]. The linkage was made by utilising the Swedish national identity number ensuring a unique number sequence that all Swedish citizens are identified by.

Estimated glucose disposal rate (eGDR)

The eGDR (mg/kg/min) was calculated as previously described according to the following formula: eGDR = 21.158 − (0.09 * WC)  −  (3.407 * HT)  −  (0.551 * HbA1c) [WC = waist circumference (cm), HT = hypertension (yes = 1/no = 0), and HbA1c = HbA1c (% DCCT)] [8].

Since the eGDR formula was developed for use in individuals with type 1 diabetes, we investigated the correlation between eGDR formula with a euglycaemic hyperinsulinaemic clamp procedure from 24 male T2D patients that have been investigated before in our lab (Additional file 1: Table S1). The correlation between clamp and eGDR were r = 0.73 (Additional file 1: Table S1; Figure S1 top).

Analysis of HbA1c was performed at local laboratories with the high-performance liquid chromatography Mono-S method and was quality-assured nationwide by regular calibration. We converted all HbA1c values to standard values according to the National Glycohaemoglobin Standardization Program [17]. Hypertension was defined as treatment with anti-hypertensive medication, or systolic blood-pressure > 140 mmHg, or diastolic blood-pressure > 90 mmHg, respectively.

Study outcomes

A flow chart of the studied patients is presented in Additional file 1: Figure S2. The main outcome was time to stroke and mortality (divided in all-cause mortality and cardiovascular mortality). Patients were studied from index date until stroke, death or end of the study (Dec 31, 2016). International Classification of Diseases codes (ICD codes) I63 and I64 were used for ischaemic stroke, and I61 to I62 for intracerebral haemorrhage, to identify all strokes. Subarachnoid haemorrhage (ICD code I60) was not included in the study. Only the first hospital admission was used for patients with several stroke episodes. For the CV death outcome, the following ICD codes were used: I20-I25 and I61-I64. The ICD codes for comorbidities are given in Additional file 1: Table S2.

Statistical analysis

The study cohort is described using standard descriptive statistics in terms of averages with standard deviation for continuous variables and counts with percentages for categorical variables. The incidence rate of all stroke (haemorrhagic stroke and ischaemic stroke), haemorrhagic stroke and ischaemic stroke was calculated as the number of events per 1000 person years and presented with 95% exact Poisson confidence intervals (CI).

The association between eGDR (mg/kg/min) was categorised as previously used cut-off levels [9, 10]: < 4 (highest grade of insulin resistance i.e., reference), 4–5.99, 6–7.99, and ≥ 8 mg/kg/min) and stroke events were illustrated using Kaplan–Meier curves and analytically assessed using three Cox regression models; unadjusted, adjusted for age and sex, and adjusted for age, sex, diabetes duration, LDL-cholesterol, HDL-cholesterol, triglycerides, lipid lowering medication, micro albuminuria, macro albuminuria, creatinine, estimated glomerular filtration rate (eGFR), retinopathy, smoking, physical activity, disposable income, marital status, education, cardiovascular morbidities, renal disorder, hyperglycaemia, amputation, dementia, psychiatric disorder and gastric bypass surgery.

The shape of the association between eGDR and stroke events was assessed using Cox regression models where the effect of eGDR was modelled using smoothing splines with 5 degrees of freedom in models also containing sex as a binary variable and a smoothing spline with 5 degrees of freedom modeling the effect of age.

The relative predictive performance for each variable in the eGDR formula was evaluated using Heller R² [18].

The association between eGDR and post stroke mortality was assessed using three Cox regression models; unadjusted, adjusted for age at the index stroke event and sex, and adjusted for sex, age at the stroke event and the last pre-stroke observations on systolic blood pressure, diastolic blood pressure, body mass index (BMI) LDL-cholesterol, HDL-cholesterol, smoking, eGFR, lipid lowering medication and anti-hypertensive treatment. P-values below 5% are regarded as indicators of statistical significance and there was no adjustment for multiple comparisons. The statistical analysis was done using R 4.0.2 and SAS 9.4

Study population and patient characteristics

A total of 104 697 individuals with T2D (women 44%) with a mean age of 62.9 years, and with a diabetes duration of 4.1 years had a baseline eGDR from index date and were included in the study. After categorising individuals according to eGDR groups a total of 24,706 (24%), 40,187 (38%), 21,042 (20%) and 18,762 (18%) had an eGDR of < 4, 4–6, 6–8 and ≥ 8 mg/kg/min, respectively. The mean age, the proportion of men, diabetes duration, HbA1c levels, blood pressure, physical inactivity, proportion of individuals with cardiovascular disease, nephropathy all decreased with increasing eGDR. Also, individuals in lower eGDR categories were more often treated with antihypertensive treatments, lipid-lowering agents, oral glucose-lowering agents and insulin (Table 1).

Association between eGDR and stroke

Event rates for stroke, i.e., all stroke (ischaemic stroke and haemorrhagic stroke), ischaemic stroke and haemorrhagic stroke, are shown in Table 2. The Kaplan–Meier estimated curves of a first stroke according to the eGDR categories are shown in Fig. 1. During a median follow-up time of 5.6 years, in total 4201 individuals with T2D had a stroke. The crude incidence rates, age-adjusted, and multivariable-adjusted risk of stroke among individuals with T2D, as categorised into different eGDR groups, are shown in Table 2. After multiple adjustments the incidence of all stroke and ischaemic stroke decreased in groups with increasing eGDR (Table 2; Fig. 2). However, for haemorrhagic stroke a non-significant difference was observed between the lowest eGDR compared to the other categories of eGDR (Table 2; Fig. 2).

Cumulative incidence of stroke in 104 697 individuals with type 2 diabetes (T2D) separated by the four categories of estimated glucose disposal rate (eGDR)

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Outcome of stroke divided into all stroke (ischaemic and haemorrhagic stroke), ischaemic and haemorrhagic strokes in 104 697 people with type 2 diabetes in Sweden, from 2004 to 2016, according to estimated glucose disposal rate (eGDR). Reference eGDR < 4 mg/kg/min

Full size image

We also analyzed the potentially non-linear association between eGDR levels and stroke risk with restricted cubic splines in a sex and age adjusted Cox regression model. As demonstrated in the (Additional file 1: Figure S3 there was a linear decrease in the risk of ischaemic stroke starting from eGDR 2 mg/kg/min.

eGDR and risk of stroke stratified by insulin treatment or no insulin treatment

In the cohort 6.4 and 8.3% were treated with insulin only and tablets and insulin, respectively. In the full model after adjusting for insulin treatment no interaction was found for the risk of all stroke p = 0.86, ischaemic stroke p = 0.78, or haemorrhagic stroke p = 0.81, respectively (Additional file 1: Figure S4). Estimates for haemorrhagic stroke were however opposite compared to estimates for all stroke and ischaemic stroke in individuals treated with insulin, although not statistically significantly different from the lowest eGDR category HRs (95% CI): 1.19 (0.63–2.22), 1.63 (0.46–5.8) and 2.67 (0.45–15.74) (Additional file 1: Figure S4).

Explained variance of the variables for stroke in the eGDR formula

The estimated explained relative risk (R² ± SD) for each variable in the eGDR formula for the risk of stroke was highest for hypertension (0.045 ± 0.0024), followed by HbA1c (0.013 ± 0.0014), and waist (0.006 ± 0.0009) (Additional file 1: Table S3).

Association between eGDR and mortality after stroke

The event rates for all-cause mortality and cardiovascular mortality are shown in Table 3. During a mean follow up time of 5.6 years in total 3.1% (3232 of 104 697) patients died. According to eGDR categories < 4, 4–6, 6–8 and ≥ 8 mg/kg/min, death occurred, relative to a stroke in 783 (36.6%), 1563 (41.9%), 633 (43.5%) and 253 (37.5%). After multiple adjustments all-cause mortality and cardiovascular mortality rate, after stroke, was lower in individuals categorised in higher eGDR groups (Table 3). HRs (95% CI) for individuals in the highest eGDR category were for all-cause mortality: 0.68 (0.53–0.89) and for cardiovascular mortality 0.65 (0.45–0.93), respectively, compared to individuals in the lowest eGDR category (Table 3).

eGDR calculated using body mass index (eGDR_BMI)

We also calculated eGDR using BMI instead of waist circumferences, i.e., eGDR_BMI (see text, Additional file 1) in which 205 482 individuals with T2D (Additional file 1: Table S4) were included. The correlation between clamp and eGDR_BMI was r = 0.69 (Additional file 1: Table S1; Figure S1 bottom). All analyses were repeated, and the results are shown in (Additional file 1: Tables S5 and S6 and Figures S5 and S6, respectively. The results were very similar to the results from the main analyses using eGDR from waist circumference. After multiple adjustment the risk of a stroke decreased with increasing eGDR_BMI HRs (95% CI): 0.72 (0.67–0.76), 0.56 (0.52–0.61) and 0.39 (0.35–0.44), compared with the reference eGDR_BMI < 4 (Additional file 1: Table S5). There was the same increased risk of mortality after a stroke by analysing eGDR_BMI (Additional file 1: Table S6). The estimated explained relative risk for stroke (R² ± SD) was higher for BMI (0.021 ± 0.00172) compared to waist (0.006 ± 0.0009) (Additional file 1: Table S3).

This nationwide study, including individuals with T2D, shows that higher eGDR (decreased insulin resistance) was associated with lower risk of stroke and death. The association was independent of clinical characteristics and other identified risk factors for stroke and mortality.

The explained attributable relative risk of a stroke, for each factor in the eGDR formula, was highest for hypertension followed by BMI, HbA1c, and waist circumference, all well known risk factors for stroke [19]. Other known stroke risk factors such as: atrial fibrillation, heart failure, smoking, macrovascular complications, and socioeconomic factors, could also have contributed to the higher risk of stroke observed in the present study [5, 20]. After adjustment for these and a wealth of other risk factors for stroke there was still a monotonic lower risk of stroke and death in the higher eGDR categories compared to the lowest eGDR category, suggesting eGDR as an important risk marker for stroke in individuals with T2D.

Since hypertension is one of the strongest risk factors for stroke, both in people with or without diabetes [19, 21] our findings are not unique and not unexpected. This was also reflected by the attributable risk of the variables in the eGDR formula in which hypertension was most important. In a recent meta-analysis it was shown that a 10 mmHg decrease in systolic blood pressure is associated with a significant decreased risk of stroke people with diabetes [22]. This was also demonstrated in the recent published ONTARGET study whereas individuals with diabetes and cardiovascular risk factors showed a reduction in stroke with a systolic blood pressure up to ≤ 115 mmHg [23]. These studies simply demonstrate the importance to treat hypertension avoiding a stroke. In the INTERSTROKE case–control study, which was launched to investigate the potentially modifiable risk factors associated with stroke, ten strong risk factors for stroke were identified and collectively associated with 90% of patients’ attributable risk [19]. Hypertension had a greater association with haemorrhagic stroke, than with ischaemic stroke, whereas smoking, diabetes, apolipoproteins and cardiovascular disease were more often associated with ischaemic stroke [19]. In the present study, the proportion of stroke events were almost 8 to 9-folded higher for ischaemic stroke, then for haemorrhagic stroke, making the interpretation for the association between risk factors and the risk of haemorrhagic stroke less reliable (less events) compared to ischaemic stroke. However, by using BMI instead of waist circumference in the eGDR formula the number of patients and events were doubled demonstrating the same monotonic pattern for haemorrhagic stroke as for ischaemic stroke.

It was recently shown from the NDR that T2D individuals who had five predefined cardiovascular risk factors, i.e., HbA1c levels, LDL-cholesterol levels, albuminuria, smoking and elevated blood pressure within the clinical target range were not at a higher risk of stroke as for the general population [24]. By using ancillary analyses the strength of the association was estimated among a wealth of risk factors and the risk of cardiovascular outcome, including stroke and mortality. In that study the strongest association for stroke was observed in T2D people with poor glycaemic control, followed by elevated systolic blood pressure, longer duration of diabetes, physical inactivity and atrial fibrillation. Recently, our group confirmed the above results demonstrating a robust association between poor glycaemic control and risk of stroke in individuals with T2D [4]. In the present study, individuals in the lowest eGDR category had a mean HbA1c level of 62 mmol/mol compared to 47 mmol/mol in individuals in the highest eGDR category; since hyperglycaemia is one modifiable risk factor for stroke achievement of good glycaemic control should be strived for to minimise this complication [4].

Obesity has been shown to increase the risk of multiple disease conditions including stroke [25]. In contrast, a survival advantage among individuals with higher BMI has also been suggested for stroke, i.e., the so-called obesity paradox, and whether obesity is an established risk factor for stroke is still debated [26]. In a large observational study among people with type 1 diabetes however no such paradox exists [27]. It has also been reported among overweight and obese T2D individuals a considerably independent increased risk for stroke and total mortality [28]. Increased waist-to-hip ratio was also a strong risk marker in the INTERSTROKE case–control study [19]. Since, waist circumference reflects central obesity and independently is associated with insulin resistance and cardiovascular disease, we used this variable in the main eGDR analysis. After replacement with BMI, instead of waist circumference in the eGDR formula, there was the same robust monotonic decrease in a stroke event and mortality thereof above reference eGDR category, and the estimated explained attributable risk was even higher for BMI compared to waist circumference. Even though an obesity paradox may exist it has not been proven in large observational studies (like the present), whereas both waist circumference and BMI associate to the risk of stroke.

Although our data from euglycaemic hyperinsulinaemic clamps, to some extent correlated to the eGDR formula used for individuals with type 1 diabetes [29], we cannot tell whether insulin resistance contributes for the excess risk of stroke or mortality observed in the present study. The impact of insulin resistance on cardiovascular disease is not easy to determine since it is clustering with several other traditional risk factors, e.g., hypertension, obesity, elevated triglycerides, low levels of HDL-cholesterol and hyperglycaemia [10]. Interestingly, it has been evaluated in a mathematical model that preventing insulin resistance would yield as much as 40% prevention of cardiovascular disease in young adults [6]. Even though insulin resistance is suggested the most important single risk factor for cardiovascular disease, its effect is indirect mediated thorough its effect on other variables such as blood pressure, lipidaemia and glycaemia [6]. When we adjusted for variables known to be linked between insulin resistance and cardiovascular complications, eGDR above reference was strongly associated with a reduced risk of stroke and death thereof in a stepwise manner. Insulin therapy, often needed to combat hyperglycaemia in T2D individuals, has been proven safe in large randomised controlled cardiovascular outcome trials [30, 31]. In contrast, some large observational studies have come to another conclusion, suggesting an association between insulin therapy in people with T2D and cardiovascular disease or premature death [32]. In the present study there was no interaction between insulin therapy and stroke. The estimates for haemorrhagic stroke in the insulin treated individuals did however not follow the pattern as for ischaemic stroke, which simply can be explained by the very small number of events in this group.

The strength of this study was its unique nationwide coverage with a large cohort of T2D individuals; and a long follow up-time with accurate and register data with high external and internal validity. However, there are some limitations; eGDR is a measure of insulin resistance developed for individuals with type 1 diabetes, although the correlation between euglycaemic hyperinsulinaemic clamp and eGDR were good (however only tested for men) we cannot conclude that eGDR can be replaced with the gold standard clamp technique. Another limitation is that we lack information of medical therapy for secondary prevention, nor did we in this study have any data on the use of antidiabetic medication such as incretins and sodium glucose transporter-2 inhibitors which has been proven beneficial on cardiovascular mortality, and may have different impact on the risk of stroke. As in any observational study, we cannot rule out that residual confounding factors affected our findings.

In conclusion we found that in individuals with T2D a low eGDR, a simple measure of insulin resistance, was associated with an increased risk of a stroke and mortality. Consequently, insulin resistance seems to increase the risk for stroke in type 2 diabetes, and eGDR may be used as a risk marker for stroke and death.

The datasets analysed during the current study are available from the corresponding author on reasonable request.

BMI:

Body mass index

CI:

Confidence interval

CHD:

Coronary heart disease

DPP4i:

Dipeptidyl peptidase 4 inhibitors

eGDR:

Estimated glucose disposal rate

GLP-1:

Glucagon-like peptide-1

HbA1c:

Glycosylated haemoglobin A1c

HR:

Hazard ratio

ICD:

International Classification of Disease

IPR:

In patient registry

IQR:

Interquartile range

LISA:

Longitudinal integration database for health insurance and job market studies register

MACE:

Major adverse cardiac event

MI:

Myocardial infarction

NDR:

National diabetes register

NPR:

Swedish national patient register

OR:

Odds rate

SD:

Standard deviation

SLGT2i:

Sodium glucose transporter-2 inhibitors

T2D:

Type 2 diabetes

TN is funded by the Hjärt-Lungfonden (grant 20190298) and ALF agreement between Stockholms Läns Landsting and Karolinska Institutet (grant 20170120). V.D. and C.P. are funded by the Swedish Research Council, and by the European Association for the Study of Diabetes.

Open access funding provided by Karolinska Institute. TN is funded by the Hjärt-Lungfonden (grant 20190298) and ALF agreement between Stockholms Läns Landsting and Karolinska Institutet (grant 20170120). V.D. and C.P. are funded by the Swedish Research Council, and by the European Association for the Study of Diabetes.

Authors and Affiliations

1. Department of Clinical Science and Education, Karolinska Institutet, Södersjukhuset, 11883, Stockholm, Sweden

   Alexander Zabala, Vladimer Darsalia, Cesare Patrone & Thomas Nyström

2. Institute of Medicine, University of Gothenburg, Gothenburg, Sweden

   Marcus Lind, Ann-Marie Svensson & Björn Eliasson

3. Department of Medicine, NU Hospital Group, Uddevalla, Sweden

   Marcus Lind

4. Centre of Registers in Region Västra Götaland, Gothenburg, Sweden

   Ann-Marie Svensson & Stefan Franzén

5. Department of Molecular Medicine and Surgery, Karolinska Institutet, Stockholm, Sweden

   Magnus Jonsson

6. Department of Vascular Surgery, Karolinska University Hospital, Stockholm, Sweden

   Magnus Jonsson

Contributions

All authors participated in the research design. SF performed the data management and statistical analyses after discussion with all authors. All authors participated in data interpretation. AZ and TN wrote the first draft of the manuscript, and all authors took final responsibility for the decision to submit for publication. TN is the guarantor of this paper.

Corresponding author

Correspondence to Alexander Zabala.

Ethical approval and consent to participate

All patients have consented to being reported in NDR. No individual consent is required for inclusion in this study, according to Swedish law. This nationwide registry based retrospective nationwide cohort study was approved by the regional ethics committee in Gothenburg, Sweden (EPN Dnr 776-14).

Consent for publication

Not applicable.

Competing interests

TN has received unrestricted grants from AstraZeneca and NovoNordisk and has served on national advisory boards of Amgen, Novo Nordisk, Sanofi-Aventis, Eli Lilly, MSD and Boehringer Ingelheim. ML has received research grants from DexCom and Novonordisk and been consultant for Astra Zeneca, Boheringer Ingelheim, DexCom, Eli Lilly, MSD and Novonordisk.

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