Objective: To evaluate the cost-effectiveness of adding relevant second-line agents to metformin for cardiovascular disease reduction in a type 2 diabetes population using post-marketing observational data. Methods: First, a retrospective national propensity score matched cohort was determined using the Taiwan National Health Insurance Research Database 2010-2015. Five metformin-based dual therapy groups were identified: metformin plus sulfonylureas, metformin plus acarbose, metformin plus meglitinides, metformin plus thiazolidinediones, and metformin plus DPP4 inhibitors. Metformin plus sulfonylureas was chosen as the reference group due to its conventional second-line therapy status. In our economic analysis, effectiveness measure included major adverse cardiovascular events and mortality, while cost measure considered direct medical cost. A Markov chain model was applied to project clinical and economic outcomes over a lifetime horizon, discounted at 3.5% per annum. An incremental cost-effectiveness ratio was determined. Sensitivity analysis was carried out to assess uncertainty in base-case assumptions. Results: In the base-case analysis, all treatments reduced costs, and all treatments except MET-MEG increased life-years. Thus MET-ALPHA, MEG-TZD, and MET-DPP4i were cost-effective compared to MET-SU. MET-ALPHA gained incremental benefits of 0.54 life-years at a cost-saving of $6,146 for an ICER of -$11,283 per LY. MET-TZD achieved incremental benefits of 2.41 life-years with a cost-saving of $2,085 for an ICER of -$8,64 per LY. MET-DPP4i achieved incremental benefits of 0.94 life-years at a cost-savings of $3,161 for an ICER of -$3,372 per LY. Results were consistent across a range of sensitivity analyses. Conclusion: This study provided empirical economic evidence to inform the choice of second-line agents, especially when CVD is considered important. Under present conditions in Taiwan, we would give preference to adding novel second-line agents to metformin for those who fail monotherapy, as compared to conventional MET–SU therapy. Antidiabetic drugs with superior cardiovascular profiles (such as DPP4 inhibitors, thiazolidinediones, and alpha-glucosidase inhibitors) demonstrate modest life-year gains and lower costs over time. We anticipate an appropriate use of these cost-effective treatment options will help payers and physicians mitigate the growing burden of diabetes.