Aim: Proven benefits of hormone replacement therapy (HRT) include relief of vasomotor symptoms and vaginal atrophy and prevention and treatment of osteoporosis. Therefore, HRT given as either unopposed estrogen replacement therapy (ERT) or estrogen plus progestin gained widespread popularity in the United States since 1960s. The Women's Health Initiative (WHI) trial of estrogen plus progestin vs. placebo was stopped early, after a mean 5.6 years of follow-up, because the overall health risks of hormone therapy exceeded its benefits. The Women’s Health Initiative Estrogen-Alone trial comparing conjugated equine estrogens with placebo was stopped early because of an increased stroke incidence and no reduction in risk of coronary heart disease. Preliminary results suggesting possible reduction in breast cancers which are not consistent with the findings of some observational studies warranted more detailed analysis. Because female hormones are reimbursed under the National Health Insurance program in Taiwan, it is possible to access and analyze nationwide data for these drugs. The purposes of this study were to estimate the effect of hormone replacement therapies (HRT) on the risk of incidence of breast cancer in women in Taiwan. Method: We used the 1,000,000 random sampling from the National Health Insurance Research Database (NHIRD) during 1997-2008 in our study. After excluded male, aged fewer than 20 and above 80, women who had cancer or had breast cancer medication previously, we had totally 305,633 women. In order to avoid the effect of Chinese herbal product, we also excluded 239,910 women who ever used it. At last, we recruited 65,723 who used estrogen alone, progesterone alone, estrogen plus progesterone and women used neither hormone nor Chinese herbal products were recruited into our study. The risk of hormone utilization was estimated by Cox model. Results & Discussion: Among 2,798 women who have used solely estrogen plus progestin during study period, 45 newly breast cancer were diagnosed after taking estrogen plus progestin. Comparing to 76 newly diagnosed breast cancers among 5,156 women who have used unopposed estrogen during the same study period, significant higher estimated hazard rate of estrogen plus progestin users was found in present study. Women used combination of estrogen and progesterone in the last year were under the higher risk (HR: 8.71, 95%CI, 5.50-13.82) than estrogen-only (HR: 2.04, 95%CI, 1.37-3.06). Of all breast cancer women among estrogen plus progestin users, 23 (51%) of them were diagnosed at age between 55 and 79 years. Further analyses found that the significant association between the current use of estrogen plus progestin and the risk of breast cancer incidence among women aged between either 20 to 79 years or 55 to 79 years who were less likely to use oral pills. The data also demonstrated that discontinued exposure to estrogen plus progestin for half a year will significant decrease the risk of breast cancer among both women of reproductive age and 55 to 79 years of age, and the trend for lower risk was observed for women discontinuing exposure for longer period. This observation suggests a role for cumulative exposure of estrogen plus progestin on breast cancer risk. The positive association between ERT use and the increase of breast cancer occurrence was also found. In addition, the trends across categories of usage status appeared to be the longer discontinued ERT use before breast cancer was diagnosed are significant associated with the lower risk of breast cancer, indicating a positive relationship exists between excessive exposure of unopposed estrogen and breast cancer. The results of present study strongly support an added impact of progestin on the breast cancer risk associated with ERT. Various type of HRT were prescribed either following the updated guidelines on the use of HRT or after careful clinical judgment based on well informed about the potential benefit and perceived risks of HRT by well-trained qualified physicians resulting in the clinical performance that women use combined estrogen-progestin had significant higher breast cancer incidence than those use unopposed estrogen. Conclusions: This study provides strong evidence that the addition of a progestin to HRT enhances markedly the risk of breast cancer relative to estrogen use alone in Taiwan. These findings have important implications for the risk–benefit equation for HRT in women using estrogen plus progestin.