Table 2.
Primary and secondary outcomes
| Outcome measure: | |
|---|---|
| Primary outcome | |
| To compare the effect of exenatide versus biphasic insulin aspart 30 on glucose variability in T2DM patients inadequately controlled with metformin monotherapy. | Absolute change of MAGE from baseline to Week 16 |
| Secondary outcome | |
| To compare the effect of exenatide versus biphasic insulin aspart 30 on inflammatory and oxidative stress markers, HbA1c, weight, risk of hypoglycemia and cardiovascular risk markers. | HbA1c at baseline and Week 16 |
| Hours of hypoglycemia assessing by CGMS at baseline and Week 16 | |
| SMBG at baseline and Week 16 | |
| Blood pressure and lipids at baseline and Week 16 | |
| Body weight, BMI and WC at baseline and Week 16 | |
| Inflammatory markers (MCP-1, hs-CRP) at baseline and Week 16 | |
| Urinary albumin at baseline and Week 16 | |
| Safety outcome | |
| To evaluate the safety and tolerability of exenatide in relation to biphasic insulin aspart 30. | Adverse events/serious adverse events |
| Vital signs | |
| Clinical hypoglycemia | |
| Collection of clinical chemistry/hematology parameters | |
| Electrocardiogram | |
T2DM, type 2 diabetes mellitus; MAGE, mean amplitude of glycemic excursion; CGMS, continuous glucose monitoring system; BMI, body mass index; WC, waist circumference; MCP-1, monocyte chemotactic protein-1; hs-CRP, high-sensitivity C-reactive protein