Replication and cross-validation of type 2 diabetes subtypes based on clinical variables: an IMI-RHAPSODY study

Data from 15,940 individuals with type 2 diabetes from three cohorts, DCS (Netherlands), GoDARTS (Scotland) and ANDIS (Sweden), were used in this cross-sectional study within the RHAPSODY consortium. RHAPSODY (Risk Assessment and ProgreSsiOn of Diabetes, https://​imi-rhapsody.​eu) is an Innovative Medicine Initiative project and one of the aims is to improve the segmentation of people with type 2 diabetes, supporting the implementation of novel strategies for diabetes prevention and treatment. Inclusion criteria for RHAPSODY were age of diagnosis ≥35, clinical data available within 2 years after diagnosis, GAD negative, no missing data in one of the five clinical measures used for clustering and the presence of genome-wide association study (GWAS) data.

Clustering was performed on five risk factors for type 2 diabetes progression [12]: age at first visit (years); BMI (kg/m²); HbA_1c (mmol/mol); HDL-cholesterol (mmol/l); and C-peptide (nmol/l). C-peptide was included as a proxy of insulin resistance and, to some extent, beta cell function (electronic supplementary material [ESM] Table 1) in absence of fasting glucose in GoDARTS (preventing the use of HOMA). HDL-cholesterol levels were included as lower HDL-cholesterol has previously been recognised as a risk factor for time to insulin requirement [12]. Clustering was performed separately in each cohort and stratified by sex. Clusters were defined based on k-means using the kmeansruns function in the R package fpc (https://​cran.​r-project.​org/​web/​packages/​fpc/​index.​html). The optimal number of clusters was determined using the gap statistic across the three cohorts [13], this being defined as the point where the curve of the gap statistic vs the number of clusters flattened, with little added value of increasing the number of clusters. The stability of the clusters was assessed in two ways. The clusters identified here in ANDIS using C-peptide instead of HOMA2 were compared with their previously published clusters based on HOMA2 [1]. Second, identified clusters were cross-validated between cohorts to assess their stability. For this, individuals from cohort A were assigned to clusters based on the cluster centres of each of the clusters identified in cohort B. This approach will quantify the probability that an individual in cohort A will be assigned to the same cluster, but based on the clustering model for cohort B. Next, predicted clusters in cohort A based on the clusters of cohort B were compared with the ‘real’ clusters of cohort A. This was done for each of the three pairwise comparisons (DCS–GoDARTS, DCS–ANDIS, GoDARTS–ANDIS). Agreement between clusters was assessed based on the specificity and sensitivity.

Time to insulin requirement was defined as the period until an individual started sustained (more than 6 months in duration) insulin treatment or required insulin, defined as ≥2 HbA_1c measurements >69 mmol/mol (8.5%) at least 3 months apart and when on ≥2 non-insulin glucose-lowering drugs. Cox proportional hazard models were used where one cluster was tested against the other clusters as a reference group in each individual cohort. Thereafter, results were meta-analysed using random effects meta-analysis using the metagen function from the meta package (https://​cran.​r-project.​org/​web/​packages/​meta/​index.​html). Analyses were performed using R statistics (version 3.6.2; https://​www.​r-project.​org/​). Figures were produced using the R packages ggplot2 (v3.3.0) (https://​cran.​r-project.​org/​web/​packages/​ggplot2/​index.​html) and omicCircos (v1.22.0) (http://​www.​bioconductor.​org/​packages/​release/​bioc/​html/​OmicCircos.​html).

In this cross-sectional study, 15,940 individuals from three cohorts were included, for which baseline characteristics are given in Table 1. The characteristics of the three cohorts were generally comparable, with the majority male participants and an average age of around 60 years. Individuals were clustered based on age, BMI, HbA_1c, C-peptide and HDL-cholesterol. The optimal number of clusters was based on the gap statistic across the three cohorts. In GoDARTS the optimal number of clusters was five, with lower gap statistics from six onwards. In DCS and ANDIS, the increase in gap statistic showed a clear stabilisation after five clusters. Therefore, we considered five the most optimal number of clusters (ESM Fig. 1a). The first cluster comprised 13–17% of the individuals included. It was characterised by high HbA_1c, but, compared with the other clusters, participants were younger with lower BMI, C-peptide and HDL-cholesterol levels. When compared with the original clusters in ANDIS [1], this cluster was most similar to the SIDD cluster with a sensitivity (SEM) of 90.7% (CI 88.4%, 92.6%; Fig. 1, ESM Fig. 1b) [1]. Between 9% and 22% of individuals clustered to a cluster with high C-peptide levels and age, but relatively lower HbA_1c and HDL-cholesterol levels, suggestive of insulin resistance. Indeed, compared with the ANDIS clusters, this cluster resembled most the SIRD cluster with an SEM of 92.4% (CI 89.7%, 94.6%; Fig. 1, ESM Fig. 1b) [1]. The third cluster comprised participants with high BMI and the youngest age and relatively lower levels of HbA_1c and HDL-cholesterol. It was most similar to the originally described MOD cluster with an SEM of 80.6% (CI 78.4%, 82.7%) and comprised 18–23% of the individuals included in the study. The fourth and fifth clusters were most similar to the MARD cluster and showed a combined sensitivity of 79.1% (CI 77.5%, 80.6%) against the MARD cluster in ANDIS (Fig. 1, ESM Fig. 1b) [1]. The fourth cluster, which was also the largest, encompassing 29–35% of the individuals, showed no extreme characteristics and was termed mild diabetes (MD). The fifth cluster was characterised by higher age and HDL-cholesterol and was termed mild diabetes with high HDL-cholesterol (MDH), and comprised 16–19% of the individuals (Fig. 1). Between male and female participants there were small differences in characteristics, but the overall differences between clusters were similar across both sexes (ESM Fig. 2).

To assess the stability across cohorts, clusters were cross-validated between cohorts. Clusters generally cross-validated well between the three cohorts (ESM Fig. 3, ESM Table 2). The SIDD and MDH clusters showed the highest sensitivity of the five clusters identified, ranging from 85.6% (CI 83.5%, 87.6%) to 97.1% (CI 94.8%, 98.5%) in SIDD and from 73.3% (CI 69.5%, 77.0%) to 92.9% (CI 91.3%, 94.3%) in MDH (ESM Fig. 3, ESM Table 2). The SIRD and MD clusters performed generally worst in terms of sensitivity, with sensitivities ranging from 36.1% (CI 32.3%, 39.9%) to 92.3% (CI 90.1%, 94.2%) in SIRD and from 40.8% (CI 38.9%, 42.7%) to 78.1% (CI 75.9%, 80.2%) in MD. Individuals clustered to SIRD were classified as MD and vice versa (ESM Fig. 3, ESM Table 2). The sensitivity of the MOD cluster ranged from 55.0% (CI 52.6%, 57.3%) to 93.2% (CI 91.5%, 94.7%).

Next, we assessed differences between clusters in terms of progression towards insulin initiation or requirement. As expected, the SIDD cluster showed the fastest progression (HR 3.40 [CI 1.72, 6.72]) compared with the other clusters (Table 2, ESM Fig. 4). The SIRD group showed slower progression (0.59 [0.46, 0.76]). The clusters MD and MDH also showed differences in their progression, where MDH showed the slowest progression compared with the other clusters (0.44 [0.33, 0.59]), also slower than MD (0.81 [0.63, 1.06]).

In the current study, clusters were identified in three cohorts, based on five different clinical characteristics. We show that clusters based on random or fasted C-peptide instead of HOMA2 measures resemble those based on HOMA2 measures. By adding HDL-cholesterol, we identified one additional cluster with mild characteristics. Cross-validation between cohorts showed that there was generally a good resemblance between cohorts. Together, our results show that the clustering is generally stable across cohorts, and also when the clustering includes C-peptide instead of HOMA measures. The novel MDH cluster represents a group of people with mild diabetes and very low risk of glycaemic deterioration towards insulin requirement.