OBJECTIVES: Cardiovascular events associated with oral hyperglycemic agents (OHA) have raised significant safety concerns. This study aims to assess whether there is an association between dipeptidyl peptidase-4 (DPP-4) inhibitors, a new class of OHA, and the risk of cardiovascular events in type 2 diabetic patients with or wihout chronic kidney disease (CKD). METHODS: The retrospective cohort study was conducted using the National Health Insurance Research Database (NHIRD) in Taiwan. From the NHIRD, we identified patients diagnosed as type 2 diabetes mellitus. We further selected those who received OHA between March 1st, 2009 and December 31st, 2012 as our study subjects and classified them into the CKD cohort and the non-CKD cohort. Within each cohort we then divided patients as two groups, the DPP-4 inhibitor (DPP-4i) users and non-DPP-4 inhibitor (non-DPP-4i) users . The two groups were 1:1 matched by propensity score to attenuate potential selection bias. Outcomes of interest included a composite endpoint of ischemic stroke, myocardial infarction and cardiovascular death (MACE) and hospitalization for heart failure (hHF). COX proportional hazard models were used to examine the association between DPP-4 inhibitor and outcomes of interest. RESULTS: Between March 2009 and December 2012, we identified a total of 37,641 and 87,604 type 2 diabetic patients with and without CKD, respectively. 12,821 patients in the CKD cohort and 19,821 patients in the non-CKD cohort were exposed to DPP-4 inhibitors, and 24,792 patients in the CKD cohort and 67,732 patients in the non-CKD cohort were not. After propensity score matching, we identified 8,213 pairs of CKD patients and 12,313 pairs of non-CKD patients for analysis. In the CKD cohort, exposure to DPP-4 inhibitors are associated with a 25% increase risk of hHF (DPP-4i vs. non-DPP-4i incidence/1000 person-year: 15.0 vs. 9.9，HR=1.25; 95% CI 1.01-1.54, p= 0.037) but not with the risk of MACE (HR=0.89, p=0.144). When further stratified according to dialysis status, only those not undergoing dialysis show an increase risk of hHF associated with DPP-4 inhibitors use. On the contrary, exposure to DPP-4 inhibitors are associated with a lower risk of MACE (DPP-4i vs. non-DPP-4i incidence/1000 person-year: 9.8 vs. 12.6，HR=0.73; 95% CI 0.61-0.87, p= 0.0007), but not the risk of hHF (HR=1.09, p=0.631) in the non-CKD cohort. The decrease risk of MACE in non-CKD population is mainly contributed by a decrease risk of ischemic stroke (DPP-4i vs. non-DPP-4i incidence/1000 person-year: 7.4 vs. 10.0，HR=0.68; 95% CI 0.55-0.84, p= 0.0003) related to exposure of DPP-4 inhibitors. CONCLUSIONS: Our study shows that exposure to DPP-4 inhibitors is associated with a higher risk of hHF but not the risk of MACE in type 2 diabetic patients with CKD. However, for type 2 diabetic patients without CKD, DPP-4 inhibitors exposure is associated with a lower risk of MACE and ischemic stroke, but not with the risk of hHF. Therefore, we recommended that for type 2 diabetic patients with CKD, especially those not undergoing dialysis, DPP-4 inhibitors should be substituted with other antidiabetic agents (ADA) such as relatively short-acting sulfonylureas (SFUs), meglitinides or insulin. For type 2 diabetic patient without CKD, we recommended the use of DPP-4 inhibitors as second-line therapy, if not otherwise contraindicated. Future study with more comprehensive lab data should be warranted.