Effect of the glucagon-like peptide-1 analogue liraglutide on coronary microvascular function in patients with type 2 diabetes – a randomized, single-blinded, cross-over pilot study

We assessed 621 patients who were followed for type 2 diabetes in outpatient clinics for eligibility (Figure 3). 213 patients were excluded due to co-morbidity, primarily previous CAD (37%, including AMI, PCI and CABG), reduced renal function (13%) and gastrointestinal disease (12%, including inflammatory bowel disease, previous pancreatitis and gastric bypass). Eligible patients (n = 81) were invited to participate. Of these, 56 declined. The main reason for reluctance to participating in the study was the concern for potential side-effects to the test drug liraglutide (Victoza®). Twenty-four patients were randomized, 14 to sequence 1 and 10 to sequence 2. During the follow up period from 15.05.2013 to 15.04.2014 one patient was lost to follow up and three patients withdrew due to sustained gastrointestinal side-effects to the liraglutide treatment in sequence 1. There were no withdrawals in sequence 2. Liraglutide was generally well tolerated and side-effects were transient with duration of approximately two weeks. Background therapy needed readjustment during liraglutide treatment in 3 out of the 4 patients receiving both metformin and SU. In one case, SU dosage was halved and in two cases SU was paused during liraglutide treatment due to HbA1c levels indicating risk of hypoglycaemia. No incidents of hypoglycaemia were observed. Three patients developed angina-like symptoms and were referred to either stress echocardiography or CT angiography to rule out obstructive CAD. None of these tests came out positive and the patients continued the study protocol. In both sequences, a total of 10 patients received the full 10 weeks liraglutide treatment.

Table 1 describes baseline characteristics and echocardiographic data of the two sequences and the total study population. Participants were predominantly male (75%), with a mean age of 57 ± 9 years, were obese (BMI 33.1 ± 4.4) and had a mean HbA1c of 52.8 ± 8.2 mmol/mol. There were a high percentage of known cardiac risk factors such as hypertension (80%) and dyslipidaemia (95%) in the study population. Echocardiographic data showed a LVEF within the normal range (mean 54.6 ± 5.8). CFR ranged from 1.69 to 3.11 (mean 2.35 ± 0.45).

In two of the 70 echocardiographies performed the investigator was unable to identify LAD in the same segment compared to previous examinations for the same patient and recordings obtained at these two examinations were of poor quality. Thus, 2 patients were excluded from CFR assessment in sequence 1 because of unreliable comparability with previous examinations. Analysis of CFR was then carried out for 8 patients in sequence 1 and 10 patients in sequence 2. Adverse reactions to dipyridamole included flushing, headache, shortness of breath and increased heart rate, but generally dipyridamole was well tolerated. No cardiac arrhythmias were observed during the dipyridamole infusions.

Table 2 shows changes in CFR values before and after no treatment and liraglutide treatment allocation. There was no significant change in CFR during no treatment (before 2.45 ± 0.41; after 2.47 ± 0.42, p = 0.82). Liraglutide treatment caused a small increase in CFR, which was of borderline significance (before 2.25 ± 0.31; after 2.43 ± 0.39, p = 0.06).

Table 3 shows the difference between changes in CFR in the no treatment and the liraglutide treatment allocation. The difference between treatment allocations was not statistically significant (0.16, CI95% [-0.08; 0.40], p = 0.18).

Analyses were carried out for all 20 patients. There were no changes in RHI in the no treatment allocation (before 1.84 ± 0.41; after 1.87 ± 0.35, p = 0.70) or the liraglutide treatment allocation (before 1.89 ± 0.47; after 2.00 ± 0.40, p = 0.31) and no between treatment allocation difference (0.09, CI95% [-0.17; 0.36], p = 0.49) (Table 3). Furthermore, there was no effect on arterial stiffness, measured by augmentation index (AI), following liraglutide treatment compared to no treatment (0.20, CI95% [-5.7; 6.1], p = 0.95). Results were similar when examinations with a warning signal were removed (n = 6) (difference between changes in RHI in the two treatment allocations (0.19, CI95% [-0.07; 0.45], p = 0.14).

Liraglutide treatment was associated with a significant decrease in HbA1c compared with no treatment (-10.1 mmol/mol, CI95% [-13.9; -6.4], p = 0.01), a decrease in fasting plasma glucose (-2.13 mmol/L, CI95% [-3.24; -1.03], p < 0.001), a moderate weight loss (-1.9 kg, CI95% [-3.6; -0.2], p = 0.03) and a reduction in systolic blood pressure (-10 mmHg, CI95% [-17; -3], p = 0.01). Carry over effect was found for one variable, HbA1c, but taking this into the parameterization in the pkcross command, the effect of liraglutide remained significant (p = 0.01 versus p = <0.001). Please see Additional file 1 for carry over, period and sequence effect for all outcomes. There was no effect of liraglutide treatment on diastolic blood pressure (-2 mmHg, CI95% [-7; 3], p = 0.35), heart rate (0.05 bpm, CI95% [-6; 6], p = 0.97) or waist circumference (1 cm, CI95% [-2; 2], p = 0.96) compared with no treatment. Additionally, liraglutide had no effect on serum insulin (-6 μU/ml, CI95% [-34; 21], p = 0.65), serum C-peptide (31 pmol/L, CI95% [-150; 212], p = 0.73) or HOMA index (-1.6, CI95% [-3.7; 0.5], p = 0.13).