Diabetes and baseline glucose are associated with inflammation, left ventricular function and short- and long-term outcome in acute coronary syndromes: role of the novel biomarker Cyr 61

At 30 days, patients with glucose upon presentation of ≥ 11.1 mmol/L had significantly higher risk of the primary endpoint and mortality (Fig. 4). This was confirmed on univariate Cox regression analysis where a BSL ≥ 11.1 mmol/L was associated with a hazard ratio of 4.78 (95% CI 2.55–8.97; p < 0.001) for the primary endpoint at 30 days and a hazard ratio of 6.6 (95% CI 3.65–11.9; p < 0.001) for death at 30 days compared to patients with BSL < 6.0 mmol/L. After adjustment for diabetes history, the relationship between hyperglycemia and MACE remained significant with a hazard ratio of 5.21 (95% CI 2.47–10.98; p < 0.001). The hazard ratio for patients with a glucose of 6.0–11.1 mmol/L was 1.21 (95% CI 0.69–2.10).

Using landmark analysis, including only survivors at 30 days, patients with glucose ≥ 11.1 mmol/L still had significantly higher risk of MACE from 30 to 365 days (log rank p = 0.005; Fig. 4b). The rate of stroke at 30 days was significantly different between groups and was 2.24% in those with glucose ≥ 11.1 mmol/L, 0.93% with glucose 6–11.1 mmol/L and 0.14% in glucose < 6 mmol/L (p = 0.016). There was no difference between groups at either 30 days or 1 year in terms of revascularisation or bleeding.

When stratifying by infarct type (STEMI vs. NSTEMI/Unstable Angina), hyperglycemia (BSL ≥ 11.1 vs. BSL < 6.0) was predictive of outcomes at 365 days in both groups. The impact was more pronounced for STEMI patients (HR 5.64; 95% CI 2.95–10.76) compared to NSTEMI/UA patients (HR 3.02; 95% CI 1.25–7.31).

Finally, we found that the impact of hyperglycemia on outcomes was more pronounced in non-diabetic patients compared to diabetics. Non-diabetics presenting with glucose ≥ 11.1 mmol/L had a 30 day MACE rate of 21.6% (p < 0.001 compared to glucose < 6 mmol/L and 6–11.1 mmol/L), while diabetics presenting with glucose ≥ 11.1 mmol/L had a 30 day MACE rate of 10.3% (p = 0.06 compared to glucose < 6 mmol/L and 6–11.1 mmol/L). At 1 year non-diabetics presenting with glucose ≥ 11.1 mmol/L had a MACE rate of 27% (p < 0.001 compared to glucose < 6 mmol/L and 6–11.1 mmol/L), while diabetics presenting with glucose ≥ 11.1 mmol/L had a MACE rate of 21.7% (p = 0.01 compared to glucose < 6 mmol/L and 6–11.1 mmol/L).

In patients with glucose ≥ 11.1 mmol/L, levels of Cyr61 were significantly higher than those with glucose levels < 6.0 mmol/L or 6.0 mmol/L to 11.1 mmol/L (p < 0.001; Fig. 1). Furthermore levels of Cyr61 were higher across all categories of glucose for patients with STEMI while Cyr61 levels did not change significantly across glucose groups in NSTEMI/unstable angina (Fig. 5). Although both Cyr61, CRP and leucocyte count levels were higher in patients with glucose ≥ 11.1 mmol/L (Fig. 1), there was a weak negative correlation between Cyr61 and CRP (r = − 0.15; p < 0.001) levels, while a moderately positive correlation existed between Cyr61 and leucocyte count (r = 0.26; p < 0.001). There was no difference in Cyr61 levels in patients with HbA1c ≥ 8.0% compared to those with HbA1c < 8.0% (p = 0.13). On univariate analysis, patients with BSL > 11.1 mmol/L had significantly higher odds of having Cyr61 levels above the median (OR 2.79; 95% CI 1.87–4.16; p < 0.001). Given the known association between higher Cyr61 levels and STEMI [14], we adjusted for STEMI and other risk factors including age, gender, BMI, hypertension, diabetes, LDL cholesterol, LVEF, troponin T, STEMI and serum creatinine and CRP. There was still a strong relationship between hyperglycemia (as defined by BSL ≥ 11.1 mmol/L) and above median Cyr61 levels (OR 2.45; 95% CI 1.16–5.15, p = 0.018).

In terms of outcomes, we grouped Cyr61 levels into tertiles and found at 30 days using univariate cox regression analysis, a significantly higher risk of MACE in patients in the highest Cyr61 tertile (HR 2.39; 95% CI 1.28–4.47). After adjustment for STEMI, leucocyte count and glucose group, the relationship was not significant (HR 1.85; 95% CI 0.88–3.88) while there was a significant relationship between BSL ≥ 11.1 mmol/L and MACE (HR 5.55; 95% CI 2.71–11.37). At 1 year, after performing the same adjustments, there was a significant relationship between outcomes and the highest Cyr61 tertile (HR 2.22; 95% CI 1.33–3.72) as well as a persistent relationship between BSL ≥ 11.1 mmol/L and outcomes (HR 3.92; 95% CI 2.29–6.72).

Outcomes according to BMI were analysed in 2’004 patients according to 3 different classes of BMI levels. There were significant differences among BMI groups at baseline. A significantly higher proportion of diabetics (34.4% vs. 19.2%; p < 0.001) had BMI > 30 kg/m². Patients with BMI > 30 had the highest systolic (133.9 ± 23.2 mmHg) and diastolic (78.2 ± 15.1 mmHg) blood pressure in comparison to those with BMI 25–29.9 (systolic 130.2 ± 23.3, diastolic 75.9 ± 14.7 mmHg; p < 0.01) or a BMI < 25 (128.6 ± 23.2/73.9 ± 14.7 mmHg; p < 0.001). Moreover, the group with BMI > 30 showed the highest heart rate (77.4 ± 15.2 bpm; p < 0.003 vs. BMI 25–29.9, p = 0.52 vs. BMI < 25), higher CRP levels (12.5 ± 25.1 mg/L; p < 0.03 vs. BMI 25–29.9, p < 0.07 vs. BMI < 25) and the highest entry glucose levels (7.5 ± 3.1 mmol/L; p < 0.001 vs. BMI < 25, p < 0.05 vs. BMI 25–29.9) in comparison with the other groups.

There were no significant differences in the primary endpoint at 1 year between the three BMI groups (p = 0.211) (Table 2). When patients were grouped according to their history of diabetes, there was a significantly higher risk of the primary endpoint in diabetic patients with a BMI < 25 kg/m² compared to diabetic patients with BMI 25–29.9 kg/m² and BMI >=30 kg/m² (Table 2). In terms of 1-year mortality, diabetic patients with a BMI < 25 kg/m² had the highest mortality (14.3%), which was significantly different compared to the other BMI groups. There was no difference in outcomes in non-diabetics stratified by BMI groups (p = 0.065) (Table 2).